Compositions and methods for the therapy and diagnosis of ovarian cancer

ABSTRACT

Compositions and methods for the therapy and diagnosis of cancer, particularly ovarian cancer, are disclosed. Illustrative compositions comprise one or more ovarian tumor polypeptides, immunogenic portions thereof, polynucleotides that encode such polypeptides, antigen presenting cell that expresses such polypeptides, and T cells that are specific for cells expressing such polypeptides. The disclosed compositions are useful, for example, in the diagnosis, prevention and/or treatment of diseases, particularly ovarian cancer.

BACKGROUND OF THE INVENTION

[0001] 1. Field of the Invention

[0002] The present invention relates generally to ovarian cancer therapy. The invention is more specifically related to polypeptides comprising at least a portion of an ovarian carcinoma protein, and to polynucleotides encoding such polypeptides, as well as antibodies and immune system cells that specifically recognize such polypeptides. Such polypeptides, polynucleotides, antibodies and cells may be used in vaccines and pharmaceutical compositions for treatment of ovarian cancer.

[0003] 2. Description of Related Art

[0004] Ovarian cancer is a significant health problem for women in the United States and throughout the world. Although advances have been made in detection and therapy of this cancer, no vaccine or other universally successful method for prevention or treatment is currently available. Management of the disease currently relies on a combination of early diagnosis and aggressive treatment, which may include one or more of a variety of treatments such as surgery, radiotherapy, chemotherapy and hormone therapy. The course of treatment for a particular cancer is often selected based on a variety of prognostic parameters, including an analysis of specific tumor markers. However, the use of established markers often leads to a result that is difficult to interpret, and high mortality continues to be observed in many cancer patients.

[0005] Immunotherapies have the potential to substantially improve cancer treatment and survival. Such therapies may involve the generation or enhancement of an immune response to an ovarian carcinoma antigen. However, to date, relatively few ovarian carcinoma antigens are known and the generation of an immune response against such antigens has not been shown to be therapeutically beneficial.

[0006] Accordingly, there is a need in the art for improved methods for identifying ovarian tumor antigens and for using such antigens in the therapy of ovarian cancer. The present invention fulfills these needs and further provides other related advantages.

BRIEF SUMMARY OF THE INVENTION

[0007] Briefly stated, this invention provides compositions and methods for the therapy of cancer, such as ovarian cancer.

[0008] In one aspect, the present invention provides polynucleotide compositions comprising a sequence selected from the group consisting of:

[0009] (a) sequences provided in SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288;

[0010] (b) complements of the sequences provided in SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288;

[0011] (c) sequences consisting of at least 20 contiguous residues of a sequence provided in SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288;

[0012] (d) sequences that hybridize to a sequence provided in SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288, under moderately stringent conditions;

[0013] (e) sequences having at least 75% identity to a sequence provided in SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288;

[0014] (f) sequences having at least 90% identity to a sequence provided in SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288; and

[0015] (g) degenerate variants of a sequence provided in SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288.

[0016] In one preferred embodiment, the polynucleotide compositions of the invention are expressed in at least about 20%, more preferably in at least about 30%, and most preferably in at least about 50% of ovarian tumors samples tested, at a level that is at least about 2-fold, preferably at least about 5-fold, and most preferably at least about 10-fold higher than that for normal tissues.

[0017] In one aspect, the present invention provides polypeptides comprising an immunogenic portion of an ovarian carcinoma protein, or a variant thereof that differs in one or more substitutions, deletions, additions and/or insertions such that the ability of the variant to react with ovarian carcinoma protein-specific antisera is not substantially diminished. Within certain embodiments, the ovarian carcinoma protein comprises a sequence that is encoded by a polynucleotide sequence selected from the group consisting of SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288, and complements of such polynucleotides.

[0018] The present invention further provides polynucleotides that encode a polypeptide as described above or a portion thereof, expression vectors comprising such polynucleotides and host cells transformed or transfected with such expression vectors.

[0019] The present invention further provides polypeptide compositions comprising an amino acid sequence selected from the group consisting of sequences recited in SEQ ID NO:186, 200-202, 207, 209, 215, 247-249, 257-261, 269-272, 278-282, 284, 286 and 289-293.

[0020] In certain preferred embodiments, the polypeptides of the present invention are immunogenic, i.e., they are capable of eliciting an immune response, particularly a humoral and/or cellular immune response, as further described herein.

[0021] The present invention further provides fragments, variants and/or derivatives of the disclosed polypeptide sequences, wherein the fragments, variants and/or derivatives preferably have a level of immunogenic activity of at least about 50%, preferably at least about 70% and more preferably at least about 90% of the level of immunogenic activity of the ovarian carcinoma protein comprises an amino acid sequence encoded by a polynucleotide that comprises a sequence recited in any one of SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288.

[0022] Within other aspects, the present invention provides pharmaceutical compositions comprising a polypeptide and/or polynucleotide as described above and a physiologically acceptable carrier.

[0023] Within a related aspect of the present invention, the pharmaceutical compositions, e.g., vaccine compositions, are provided for prophylactic or therapeutic applications. Such compositions generally comprise an immunogenic polypeptide or polynucleotide of the invention and an immunostimulant, such as an adjuvant.

[0024] The present invention further provides pharmaceutical compositions that comprise: (a) an antibody or antigen-binding fragment thereof that specifically binds to a polypeptide of the present invention, or a fragment thereof; and (b) a physiologically acceptable carrier.

[0025] Within further aspects, the present invention provides pharmaceutical compositions comprising: (a) an antigen presenting cell that expresses a polypeptide as described above and (b) a pharmaceutically acceptable carrier or excipient. Illustrative antigen presenting cells include dendritic cells, macrophages, monocytes, fibroblasts and B cells.

[0026] Within related aspects, pharmaceutical compositions are provided that comprise: (a) an antigen presenting cell that expresses a polypeptide as described above and (b) an immunostimulant.

[0027] The present invention further provides, in other aspects, fusion proteins that comprise at least one polypeptide as described above, as well as polynucleotides encoding such fusion proteins, typically in the form of pharmaceutical compositions, e.g., vaccine compositions, comprising a physiologically acceptable carrier and/or an immunostimulant. The fusions proteins may comprise multiple immunogenic polypeptides or portions/variants thereof, as described herein, and may further comprise one or more polypeptide segments for facilitating the expression, purification and/or immunogenicity of the polypeptide(s).

[0028] Within further aspects, the present invention provides methods for stimulating an immune response in a patient, preferably a T cell response in a human patient, comprising administering a pharmaceutical composition described herein. The patient may be afflicted with ovarian cancer, in which case the methods provide treatment for the disease, or patient considered at risk for such a disease may be treated prophylactically.

[0029] Within further aspects, the present invention provides methods for inhibiting the development of a cancer in a patient, comprising administering to a patient a pharmaceutical composition as recited above. The patient may be afflicted with ovarian cancer, in which case the methods provide treatment for the disease, or patient considered at risk for such a disease may be treated prophylactically.

[0030] The present invention further provides, within other aspects, methods for removing tumor cells from a biological sample, comprising contacting a biological sample with T cells that specifically react with a polypeptide of the present invention, wherein the step of contacting is performed under conditions and for a time sufficient to permit the removal of cells expressing the protein from the sample.

[0031] Within related aspects, methods are provided for inhibiting the development of a cancer in a patient, comprising administering to a patient a biological sample treated as described above.

[0032] Methods are further provided, within other aspects, for stimulating and/or expanding T cells specific for a polypeptide of the present invention, comprising contacting T cells with one or more of: (i) an ovarian carcinoma polypeptide as described above; (ii) a polynucleotide encoding such a polypeptide; and/or (iii) an antigen presenting cell that expresses such a polypeptide; under conditions and for a time sufficient to permit the stimulation and/or expansion of T cells. Isolated T cell populations comprising T cells prepared as described above are also provided.

[0033] Within further aspects, the present invention provides methods for inhibiting the development of a cancer in a patient, comprising administering to a patient an effective amount of a T cell population as described above.

[0034] The present invention further provides methods for inhibiting the development of a cancer in a patient, comprising the steps of: (a) incubating CD4+ and/or CD8+T cells isolated from a patient with one or more of: (i) a polypeptide comprising at least an immunogenic portion of polypeptide disclosed herein; (ii) a polynucleotide encoding such a polypeptide; and (iii) an antigen-presenting cell that expressed such a polypeptide; and (b) administering to the patient an effective amount of the proliferated T cells, and thereby inhibiting the development of a cancer in the patient. Proliferated cells may, but need not, be cloned prior to administration to the patient.

[0035] Within further aspects, the present invention provides methods for determining the presence or absence of a cancer, preferably an ovarian cancer, in a patient comprising: (a) contacting a biological sample obtained from a patient with a binding agent that binds to a polypeptide as recited above; (b) detecting in the sample an amount of polypeptide that binds to the binding agent; and (c) comparing the amount of polypeptide with a predetermined cut-off value, and therefrom determining the presence or absence of a cancer in the patient. Within preferred embodiments, the binding agent is an antibody, more preferably a monoclonal antibody.

[0036] The present invention also provides, within other aspects, methods for monitoring the progression of a cancer in a patient. Such methods comprise the steps of: (a) contacting a biological sample obtained from a patient at a first point in time with a binding agent that binds to a polypeptide as recited above; (b) detecting in the sample an amount of polypeptide that binds to the binding agent; (c) repeating steps (a) and (b) using a biological sample obtained from the patient at a subsequent point in time; and (d) comparing the amount of polypeptide detected in step (c) with the amount detected in step (b) and therefrom monitoring the progression of the cancer in the patient.

[0037] The present invention further provides, within other aspects, methods for determining the presence or absence of a cancer in a patient, comprising the steps of: (a) contacting a biological sample obtained from a patient with an oligonucleotide that hybridizes to a polynucleotide that encodes a polypeptide of the present invention; (b) detecting in the sample a level of a polynucleotide, preferably mRNA, that hybridizes to the oligonucleotide; and (c) comparing the level of polynucleotide that hybridizes to the oligonucleotide with a predetermined cut-off value, and therefrom determining the presence or absence of a cancer in the patient. Within certain embodiments, the amount of mRNA is detected via polymerase chain reaction using, for example, at least one oligonucleotide primer that hybridizes to a polynucleotide encoding a polypeptide as recited above, or a complement of such a polynucleotide. Within other embodiments, the amount of mRNA is detected using a hybridization technique, employing an oligonucleotide probe that hybridizes to a polynucleotide that encodes a polypeptide as recited above, or a complement of such a polynucleotide.

[0038] In related aspects, methods are provided for monitoring the progression of a cancer in a patient, comprising the steps of: (a) contacting a biological sample obtained from a patient with an oligonucleotide that hybridizes to a polynucleotide that encodes a polypeptide of the present invention; (b) detecting in the sample an amount of a polynucleotide that hybridizes to the oligonucleotide; (c) repeating steps (a) and (b) using a biological sample obtained from the patient at a subsequent point in time; and (d) comparing the amount of polynucleotide detected in step (c) with the amount detected in step (b) and therefrom monitoring the progression of the cancer in the patient.

[0039] Within further aspects, the present invention provides antibodies, such as monoclonal antibodies, that bind to a polypeptide as described above, as well as diagnostic kits comprising such antibodies. Diagnostic kits comprising one or more oligonucleotide probes or primers as described above are also provided.

[0040] These and other aspects of the present invention will become apparent upon reference to the following detailed description. All references disclosed herein are hereby incorporated by reference in their entirety as if each was incorporated individually.

BRIEF DESCRIPTION OF THE SEQUENCE IDENTIFIERS

[0041] SEQ ID NO:1, 2, 5, 9, 10, 13, 16, 19, 23, 27, 28, 32, 33, 35, 38, 41-50, 52, 53, 56, 57, 63, 65, 69-72, 75, 78, 80-82, 84, 86, 89-93, 95, 97-100, 103, 107, 111, 114, 117, 120, 121, 125, 128, 132-134, 136, 137, 140, 143-146, 148-151, 156, 158, 160-162, 166-168, 171, 174-183, 185, and 193-199 are described in Tables III-VII below.

[0042] SEQ ID NO:200 is the amino acid sequence of a polypeptide encoded by the polynucleotide recited in SEQ ID NO:182;

[0043] SEQ ID NO:201 is the amino acid sequence of a polypeptide encoded by the polynucleotide recited in SEQ ID NO:182;

[0044] SEQ ID NO:202 is the amino acid sequence of a polypeptide encoded by the polynucleotide recited in SEQ ID NO:182.

[0045] SEQ ID NO:203 is the determined extended cDNA sequence for SEQ ID NO:197.

[0046] SEQ ID NO:204 is the determined extended cDNA sequence for SEQ ID NO:198.

[0047] SEQ ID NO:205 is the determined extended cDNA sequence for SEQ ID NO:199.

[0048] SEQ ID NO:206 is the determined cDNA sequence for the coding region of O568S fused to an N-terminal His tag.

[0049] SEQ ID NO:207 is the amino acid sequence of the polypeptide encoded by the polynucleotide recited in SEQ ID NO:206.

[0050] SEQ ID NO:208 is the determined cDNA sequence for the coding region of GPR39 as downloaded from the High Throughput Genomics Database.

[0051] SEQ ID NO:209 is the amino acid sequence encoded by the cDNA sequence recited in SEQ ID NO:208.

[0052] SEQ ID NO:210 is the nucleotide sequence of O1034C an ovary specific EST clone discovered using electronic subtraction.

[0053] SEQ ID NO:211 is the full length nucleotide sequence of O591S.

[0054] SEQ ID NO:212 is the sequence BF345141 which shows sequence homology with O1034C/O591S allowing for the extension of O591S.

[0055] SEQ ID NO:213 is the sequence BE336607 which shows sequence homology with O1034C/O591S allowing for the extension of O591S.

[0056] SEQ ID NO:214 is the consensus nucleotide sequence of O1034C/O591S containing 1897 base pairs.

[0057] SEQ ID NO:215 is the predicted translation of the open reading frame identified within SEQ ID NO:214 (nucleotides 260-682).

[0058] SEQ ID NO:216 is a determined 5′ DNA sequence of clone number 91226.5.

[0059] SEQ ID NO:217 is a determined 5′ DNA sequence of clone number 91227.2.

[0060] SEQ ID NO:218 is a determined 5′ DNA sequence of clone number 91230.2.

[0061] SEQ ID NO:219 is a determined 5′ DNA sequence of clone number 91231.2.

[0062] SEQ ID NO:220 is a determined 5′ DNA sequence of clone number 91238.3.

[0063] SEQ ID NO:221 is a determined 5′ DNA sequence of clone number 91239.6.

[0064] SEQ ID NO:222 is a determined 5′ DNA sequence of clone number 91240.2.

[0065] SEQ ID NO:223 is a determined 5′ DNA sequence of clone number 91241.2.

[0066] SEQ ID NO:224 is a determined 5′ DNA sequence of clone number 91242.5.

[0067] SEQ ID NO:225 is a determined 5′ DNA sequence of clone number 91243.6 .

[0068] SEQ ID NO:226 is a determined 5′ DNA sequence of clone number 91245.2.

[0069] SEQ ID NO:227 is a determined 5′ DNA sequence of clone number 91246.4.

[0070] SEQ ID NO:228 is a determined 3′ DNA sequence of clone number 91247.3.

[0071] SEQ ID NO:229 is a determined 5′ DNA sequence of clone number 91247.4.

[0072] SEQ ID NO:230 is a determined 5′ DNA sequence of clone number 91249.2.

[0073] SEQ ID NO:231 is a determined 5′ DNA sequence of clone number 91253.2.

[0074] SEQ ID NO:232 is a determined 5′ DNA sequence of clone number 91254.2.

[0075] SEQ ID NO:233 is a determined 5′ DNA sequence of clone number 91259.2.

[0076] SEQ ID NO:234 is a determined 3′ DNA sequence of clone number 91261.3.

[0077] SEQ ID NO:235 is a determined 5′ DNA sequence of clone number 91261.4.

[0078] SEQ ID NO:236 is a determined 5′ DNA sequence of clone number 91262.2.

[0079] SEQ ID NO:237 is a determined 5′ DNA sequence of clone number 91263.2.

[0080] SEQ ID NO:238 is a determined 5′ DNA sequence of clone number 91264.2.

[0081] SEQ ID NO:239 is a determined 5′ DNA sequence of clone number 91268.2.

[0082] SEQ ID NO:240 is a determined 5′ DNA sequence of clone number 91269.5.

[0083] SEQ ID NO:241 is a determined 5′ DNA sequence of clone number 91271.5.

[0084] SEQ ID NO:242 is a determined 3′ DNA sequence of clone number 91273.3.

[0085] SEQ ID NO:243 is a determined 5′ DNA sequence of clone number 91274.6.

[0086] SEQ ID NO:244 is the DNA sequence of GenBank Accession Number 18549403, which shares homology to SEQ ID NO:246.

[0087] SEQ ID NO:245 is the DNA sequence of GenBank Accession Number 10436393_FLJ14035, which shares homology to SEQ ID NO:246.

[0088] SEQ ID NO:246, also referred to as O646SgenomicContig, is a DNA (contig) sequence assembled based on a search of the publicly available databases using SEQ ID NO:243 as a query.

[0089] SEQ ID NO:247 is a amino acid sequence corresponding to the DNA sequence of GenBank Accession Number 18549403, SEQ ID NO:244.

[0090] SEQ ID NO:248 is a amino acid sequence corresponding to the DNA sequence of GenBank Accession Number 10436393_FLJ14035, SEQ IDNO:245.

[0091] SEQ ID NO:249 is a amino acid sequence corresponding to a polypeptide encoded by SEQ ID NO:246, also referred to as O646GenomicContig_MajorORF.

[0092] SEQ ID NO:250 is the DNA sequence of GenBank Accession Number 3980529, which shares homology to SEQ ID NO:262.

[0093] SEQ ID NO:251 is the DNA sequence of GenBank Accession Number 13629915, which shares homology to SEQ ID NO:262.

[0094] SEQ ID NO:252 is the DNA sequence of GenBank Accession Number 9789986, which shares homology to SEQ ID NO:262.

[0095] SEQ ID NO:253 is the DNA sequence of GenBank Accession Number 6006516, which shares homology to SEQ ID NO:262.

[0096] SEQ ID NO:254 is the DNA sequence of GenBank Accession Number 5689424, which shares homology to SEQ ID NO:262.

[0097] SEQ ID NO:255 is the DNA sequence of GenBank Accession Number 15638833, which shares homology to SEQ ID NO:262.

[0098] SEQ ID NO:256, also referred to as O646SGenomicContig, is a DNA (contig) sequence assembled based on a search of the publicly available databases using SEQ ID NO:243 as a query.

[0099] SEQ ID NO:257 is an amino acid sequence corresponding to the DNA sequence of GenBank Accession Number 13629915, SEQ IDNO:251.

[0100] SEQ ID NO:258 is an amino acid sequence corresponding to the DNA sequence of GenBank Accession Number 9789986, SEQ IDNO:252.

[0101] SEQ ID NO:259 is an amino acid sequence corresponding to the DNA sequence of GenBank Accession Number 6006516, SEQ IDNO:253.

[0102] SEQ ID NO:260 is an amino acid sequence corresponding to the DNA sequence of GenBank Accession Number 5689424, SEQ IDNO:254.

[0103] SEQ ID NO:261, also referred to as O648S_GenomicContig_ORF, is a amino acid sequence corresponding to a polypeptide encoded by SEQ ID NO:262.

[0104] SEQ ID NO:262 is the DNA sequence of GenBank Accession Number 16933560, which shares homology to SEQ ID NO:268 .

[0105] SEQ ID NO:263 is the DNA sequence of GenBank Accession Number 12053028, which shares homology to SEQ ID NO:268.

[0106] SEQ ID NO:264 is the DNA sequence of GenBank Accession Number 7638812, which shares homology to SEQ ID NO:268.

[0107] SEQ ID NO:265 is the DNA sequence of GenBank Accession Number 939922, which shares homology to SEQ ID NO:268.

[0108] SEQ ID NO:266 is the DNA sequence of GenBank Accession Number 6093230, which shares homology to SEQ ID NO:268.

[0109] SEQ ID NO:267 is the DNA sequence of GenBank Accession Number 11465000, which shares homology to SEQ ID NO:268.

[0110] SEQ ID NO:268 also referred to as O647SgenomicContig3, is a DNA (contig) sequence assembled based on a search of the publicly available databases using SEQ ID NO:234 as a query.

[0111] SEQ ID NO:269 is an amino acid sequence corresponding to the DNA sequence of GenBank Accession Number 16933560, SEQ IDNO:262.

[0112] SEQ ID NO:270 is an amino acid sequence corresponding to the DNA sequence of GenBank Accession Number 12053028, SEQ IDNO:263.

[0113] SEQ ID NO:271 is an amino acid sequence corresponding to the DNA sequence of GenBank Accession Number 7638812, SEQ IDNO:264.

[0114] SEQ ID NO:272 is an amino acid sequence corresponding to the DNA sequence of GenBank Accession Number 939922, SEQ IDNO:265.

[0115] SEQ ID NO:273 also referred to as 0645SgenomicContig2, is a DNA (contig) sequence assembled based on a search of the publicly available databases using SEQ ID NO:238 as a query.

[0116] SEQ ID NO:274 is the DNA sequence of GenBank Accession Number NM006580, also referred to as Claudin16, which shares homology to SEQ ID NO:277.

[0117] SEQ ID NO:275 is the DNA sequence of GenBank Accession Number AF152101.1, also referred to as Paracellin-1, which shares homology to SEQ ID NO:277.

[0118] SEQ IN NO:276 is the DNA sequence of GenBank Accession Number 18425237, which shares homology to SEQ ID NO:277.

[0119] SEQ ID NO:277 also referred to as O644SgenomicContig2, is a DNA (contig) sequence assembled based on a search of the publicly available databases using SEQ ID NO:240 as a query.

[0120] SEQ ID NO:278 is an amino acid sequence corresponding to the DNA sequence of GenBank Accession Number NM006580, SEQ IDNO:277.

[0121] SEQ ID NO:279 is an amino acid sequence corresponding to the DNA sequence of GenBank Accession Number AF152101.1, SEQ IDNO:275.

[0122] SEQ ID NO:280 also referred to as O644S_GenomicContig2_ORF1, is a amino acid sequence corresponding to an open reading frame of SEQ ID NO:277.

[0123] SEQ ID NO:281 also referred to as O644S_GenomicContig2_ORF2, is a amino acid sequence corresponding to an open reading frame of SEQ ID NO:277.

[0124] SEQ ID NO:282 also referred to as O644S_GenomicContig2_ORF3, is a amino acid sequence corresponding to an open reading frame of SEQ ID NO:277.

[0125] SEQ ID NO:283 is a DNA sequence of a signal peptide minus O591S fusion protein containing a N-terminal histidine tag.

[0126] SEQ ID NO:284 is a corresponding amino acid sequence of a signal peptide minus O591S fusion protein containing a N-terminal histidine tag.

[0127] SEQ ID NO:285 is a 1740 bp DNA sequence identified by BlastN search of a LifeSeq Gold database using SEQ ID NO:198 as a query.

[0128] SEQ ID NO:286 is an amino acid sequence encode by the DNA sequence set forth in SEQ ID NO:285.

[0129] SEQ ID NO:287 is the sequence for the forward primer, CBH-005, used in the amplification of O591S-A.

[0130] SEQ ID NO:288 is the sequence for the reverse primer, CBH-003, used in the amplification of O591S-A.

[0131] SEQ ID NO:289 corresponds to the amino acid sequence corresponding to residue 1-114 of SEQ ID NO:215.

[0132] SEQ ID NO:290 corresponds to the amino acid sequence corresponding to residue 1-115 of SEQ ID NO:215 (O591S).

[0133] SEQ ID NO: 291 corresponds to amino acid residues 26-55 of SEQ ID NO:215 (O591S).

[0134] SEQ ID NO:292 corresponds to amino acid residues 53-78 of SEQ ID NO:215 (O591S).

[0135] SEQ ID NO:293 corresponds to amino acid residues 103-129 of SEQ ID NO:215 (O591S).

DETAILED DESCRIPTION OF THE INVENTION

[0136] U.S. patents, U.S. patent application publications, U.S. patent applications, foreign patents, foreign patent applications and non-patent publications referred to in this specification and/or listed in the Application Data Sheet, are incorporated herein by reference, in their entirety.

[0137] The present invention is directed generally to compositions and their use in the therapy and diagnosis of cancer, particularly ovarian cancer. As described further below, illustrative compositions of the present invention include, but are not restricted to, polypeptides, particularly immunogenic polypeptides, polynucleotides encoding such polypeptides, antibodies and other binding agents, antigen presenting cells (APCs) and immune system cells (e.g., T cells).

[0138] The practice of the present invention will employ, unless indicated specifically to the contrary, conventional methods of virology, immunology, microbiology, molecular biology and recombinant DNA techniques within the skill of the art, many of which are described below for the purpose of illustration. Such techniques are explained fully in the literature. See, e.g., Sambrook, et al. Molecular Cloning: A Laboratory Manual (2nd Edition, 1989); Maniatis et al. Molecular Cloning: A Laboratory Manual (1982); DNA Cloning: A Practical Approach, vol. I & II (D. Glover, ed.); Oligonucleotide Synthesis (N. Gait, ed., 1984); Nucleic Acid Hybridization (B. Hames & S. Higgins, eds., 1985); Transcription and Translation (B. Hames & S. Higgins, eds., 1984); Animal Cell Culture (R. Freshney, ed., 1986); Perbal, A Practical Guide to Molecular Cloning (1984).

[0139] All publications, patents and patent applications cited herein, whether supra or infra, are hereby incorporated by reference in their entirety.

[0140] As used in this specification and the appended claims, the singular forms “a,” “an” and “the” include plural references unless the content clearly dictates otherwise.

[0141] Polypeptide Compositions

[0142] As used herein, the term “polypeptide” is used in its conventional meaning, i.e., as a sequence of amino acids. The polypeptides are not limited to a specific length of the product; thus, peptides, oligopeptides, and proteins are included within the definition of polypeptide, and such terms may be used interchangeably herein unless specifically indicated otherwise. This term also does not refer to or exclude post-expression modifications of the polypeptide, for example, glycosylations, acetylations, phosphorylations and the like, as well as other modifications known in the art, both naturally occurring and non-naturally occurring. A polypeptide may be an entire protein, or a subsequence thereof. Particular polypeptides of interest in the context of this invention are amino acid subsequences comprising epitopes, i.e., antigenic determinants substantially responsible for the immunogenic properties of a polypeptide and being capable of evoking an immune response.

[0143] Particularly illustrative polypeptides of the present invention comprise those encoded by a polynucleotide sequence set forth in any one of SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288; or a sequence that hybridizes under moderately stringent conditions, or, alternatively, under highly stringent conditions, to a polynucleotide sequence identified above. Certain other illustrative polypeptides of the invention comprise amino acid sequences as set forth in any one of SEQ ID NO:186, 200-202, 207, 209, 215, 247-249, 257-261, 269-272, 278-282, 284, 286, and 289-293.

[0144] The polypeptides of the present invention are sometimes herein referred to as ovarian tumor proteins or ovarian tumor polypeptides, as an indication that their identification has been based at least in part upon their increased levels of expression in ovarian tumor samples. Thus, a “ovarian tumor polypeptide” or “ovarian tumor protein,” refers generally to a polypeptide sequence of the present invention, or a polynucleotide sequence encoding such a polypeptide, that is expressed in a substantial proportion of ovarian tumor samples, for example preferably greater than about 20%, more preferably greater than about 30%, and most preferably greater than about 50% or more of ovarian tumor samples tested. at a level that is at least two fold, and preferably at least five fold, greater than the level of expression in normal tissues, as determined using a representative assay provided herein. An ovarian tumor polypeptide sequence of the invention, based upon its increased level of expression in tumor cells, has particular utility both as a diagnostic marker as well as a therapeutic target, as further described below.

[0145] In certain preferred embodiments, the polypeptides of the invention are immunogenic, i.e., they react detectably within an immunoassay (such as an ELISA or T-cell stimulation assay) with antisera and/or T-cells from a patient with ovarian cancer. Screening for immunogenic activity can be performed using techniques well known to the skilled artisan. For example, such screens can be performed using methods such as those described in Harlow and Lane, Antibodies: A Laboratory Manual, Cold Spring Harbor Laboratory, 1988. In one illustrative example, a polypeptide may be immobilized on a solid support and contacted with patient sera to allow binding of antibodies within the sera to the immobilized polypeptide. Unbound sera may then be removed and bound antibodies detected using, for example, ¹²⁵I-labeled Protein A.

[0146] As would be recognized by the skilled artisan, immunogenic portions of the polypeptides disclosed herein are also encompassed by the present invention. An “immunogenic portion,” as used herein, is a fragment of an immunogenic polypeptide of the invention that itself is immunologically reactive (i.e., specifically binds) with the B-cells and/or T-cell surface antigen receptors that recognize the polypeptide. Immunogenic portions may generally be identified using well known techniques, such as those summarized in Paul, Fundamental Immunology, 3rd ed., 243-247 (Raven Press, 1993) and references cited therein. Such techniques include screening polypeptides for the ability to react with antigen-specific antibodies, antisera and/or T-cell lines or clones. As used herein, antisera and antibodies are “antigen-specific” if they specifically bind to an antigen (i.e., they react with the protein in an ELISA or other immunoassay, and do not react detectably with unrelated proteins). Such antisera and antibodies may be prepared as described herein, and using well-known techniques.

[0147] In one preferred embodiment, an immunogenic portion of a polypeptide of the present invention is a portion that reacts with antisera and/or T-cells at a level that is not substantially less than the reactivity of the full-length polypeptide (e.g., in an ELISA and/or T-cell reactivity assay). Preferably, the level of immunogenic activity of the immunogenic portion is at least about 50%, preferably at least about 70% and most preferably greater than about 90% of the immunogenicity for the full-length polypeptide. In some instances, preferred immunogenic portions will be identified that have a level of immunogenic activity greater than that of the corresponding full-length polypeptide, e.g., having greater than about 100% or 150% or more immunogenic activity.

[0148] In certain other embodiments, illustrative immunogenic portions may include peptides in which an N-terminal leader sequence and/or transmembrane domain have been deleted. Other illustrative immunogenic portions will contain a small N- and/or C-terminal deletion (e.g., 1-30 amino acids, preferably 5-15 amino acids), relative to the mature protein.

[0149] In another embodiment, a polypeptide composition of the invention may also comprise one or more polypeptides that are immunologically reactive with T cells and/or antibodies generated against a polypeptide of the invention, particularly a polypeptide having an amino acid sequence disclosed herein, or to an immunogenic fragment or variant thereof.

[0150] In another embodiment of the invention, polypeptides are provided that comprise one or more polypeptides that are capable of eliciting T cells and/or antibodies that are immunologically reactive with one or more polypeptides described herein, or one or more polypeptides encoded by contiguous nucleic acid sequences contained in the polynucleotide sequences disclosed herein, or immunogenic fragments or variants thereof, or to one or more nucleic acid sequences which hybridize to one or more of these sequences under conditions of moderate to high stringency.

[0151] The present invention, in another aspect, provides polypeptide fragments comprising at least about 5, 10, 15, 20, 25, 50, or 100 contiguous amino acids, or more, including all intermediate lengths, of a polypeptide compositions set forth herein, such as those set forth in SEQ ID NO:186, 200-202, 207, 209, 215, 247-249, 257-261, 269-272, 278-282, 284, 286, and 289-293 or those encoded by a polynucleotide sequence set forth in any one of SEQ ID NO: 1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288.

[0152] In another aspect, the present invention provides variants of the polypeptide compositions described herein. Polypeptide variants generally encompassed by the present invention will typically exhibit at least about 70%, 75%, 80%, 85%, 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98%, or 99% or more identity (determined as described below), along its length, to a polypeptide sequences set forth herein.

[0153] In one preferred embodiment, the polypeptide fragments and variants provide by the present invention are immunologically reactive with an antibody and/or T-cell that reacts with a full-length polypeptide specifically set for the herein.

[0154] In another preferred embodiment, the polypeptide fragments and variants provided by the present invention exhibit a level of immunogenic activity of at least about 50%, preferably at least about 70%, and most preferably at least about 90% or more of that exhibited by a full-length polypeptide sequence specifically set forth herein.

[0155] A polypeptide “variant,” as the term is used herein, is a polypeptide that typically differs from a polypeptide specifically disclosed herein in one or more substitutions, deletions, additions and/or insertions. Such variants may be naturally occurring or may be synthetically generated, for example, by modifying one or more of the above polypeptide sequences of the invention and evaluating their immunogenic activity as described herein and/or using any of a number of techniques well known in the art.

[0156] For example, certain illustrative variants of the polypeptides of the invention include those in which one or more portions, such as an N-terminal leader sequence or transmembrane domain, have been removed. Other illustrative variants include variants in which a small portion (e.g., 1-30 amino acids, preferably 5-15 amino acids) has been removed from the N- and/or C-terminal of the mature protein.

[0157] In many instances, a variant will contain conservative substitutions. A “conservative substitution” is one in which an amino acid is substituted for another amino acid that has similar properties, such that one skilled in the art of peptide chemistry would expect the secondary structure and hydropathic nature of the polypeptide to be substantially unchanged. As described above, modifications may be made in the structure of the polynucleotides and polypeptides of the present invention and still obtain a functional molecule that encodes a variant or derivative polypeptide with desirable characteristics, e.g., with immunogenic characteristics. When it is desired to alter the amino acid sequence of a polypeptide to create an equivalent, or even an improved, immunogenic variant or portion of a polypeptide of the invention, one skilled in the art will typically change one or more of the codons of the encoding DNA sequence according to Table 1.

[0158] For example, certain amino acids may be substituted for other amino acids in a protein structure without appreciable loss of interactive binding capacity with structures such as, for example, antigen-binding regions of antibodies or binding sites on substrate molecules. Since it is the interactive capacity and nature of a protein that defines that protein's biological functional activity, certain amino acid sequence substitutions can be made in a protein sequence, and, of course, its underlying DNA coding sequence, and nevertheless obtain a protein with like properties. It is thus contemplated that various changes may be made in the peptide sequences of the disclosed compositions, or corresponding DNA sequences which encode said peptides without appreciable loss of their biological utility or activity. TABLE I Amino Acids Codons Alanine Ala A GCA GCC GCG GCU Cysteine Cys C UGC UGU Aspartic acid Asp D GAC GAU Glutamic acid Glu E GAA GAG Phenylalanine Phe F UUC UUU Glycine Gly G GGA GGC GGG GGU Histidine His H CAC CAU Isoleucine Ile I AUA AUC AUU Lysine Lys K AAA AAG Leucine Leu L UUA UUG CUA CUC CUG CUU Methionine Met M AUG Asparagine Asn N AAC AAU Proline Pro P CCA CCC CCG CCU Glutamine Gln Q CAA CAG Arginine Arg R AGA AGG CGA CGC CGG CGU Serine Ser S AGC AGU UCA UCC UCG UCU Threonine Thr T ACA ACC ACG ACU Valine Val V GUA GUC GUG GUU Tryptophan Trp W UGG Tyrosine Tyr Y UAC UAU

[0159] In making such changes, the hydropathic index of amino acids may be considered. The importance of the hydropathic amino acid index in conferring interactive biologic function on a protein is generally understood in the art (Kyte and Doolittle, 1982, incorporated herein by reference). It is accepted that the relative hydropathic character of the amino acid contributes to the secondary structure of the resultant protein, which in turn defines the interaction of the protein with other molecules, for example, enzymes, substrates, receptors, DNA, antibodies, antigens, and the like. Each amino acid has been assigned a hydropathic index on the basis of its hydrophobicity and charge characteristics (Kyte and Doolittle, 1982). These values are: isoleucine (+4.5); valine (+4.2); leucine (+3.8); phenylalanine (+2.8); cysteine/cystine (+2.5); methionine (+1.9); alanine (+1.8); glycine (−0.4); threonine (−0.7); serine (−0.8); tryptophan (−0.9); tyrosine (−1.3); proline (−1.6); histidine (−3.2); glutamate (−3.5); glutamine (−3.5); aspartate (−3.5); asparagine (−3.5); lysine (−3.9); and arginine (−4.5).

[0160] It is known in the art that certain amino acids may be substituted by other amino acids having a similar hydropathic index or score and still result in a protein with similar biological activity, i.e., still obtain a biological functionally equivalent protein. In making such changes, the substitution of amino acids whose hydropathic indices are within ±2 is preferred, those within ±1 are particularly preferred, and those within ±0.5 are even more particularly preferred. It is also understood in the art that the substitution of like amino acids can be made effectively on the basis of hydrophilicity. U.S. Pat. No. 4,554,101 (specifically incorporated herein by reference in its entirety), states that the greatest local average hydrophilicity of a protein, as governed by the hydrophilicity of its adjacent amino acids, correlates with a biological property of the protein.

[0161] As detailed in U.S. Pat. No. 4,554,101, the following hydrophilicity values have been assigned to amino acid residues: arginine (+3.0); lysine (+3.0); aspartate (+3.0±1); glutamate (+3.0±1); serine (+0.3); asparagine (+0.2); glutamine (+0.2); glycine (0); threonine (−0.4); proline (−0.5±1); alanine (−0.5); histidine (−0.5); cysteine (−1.0); methionine (−1.3); valine (−1.5); leucine (−1.8); isoleucine (−1.8); tyrosine (−2.3); phenylalanine (−2.5); tryptophan (−3.4). It is understood that an amino acid can be substituted for another having a similar hydrophilicity value and still obtain a biologically equivalent, and in particular, an immunologically equivalent protein. In such changes, the substitution of amino acids whose hydrophilicity values are within ±2 is preferred, those within ±1 are particularly preferred, and those within ±0.5 are even more particularly preferred.

[0162] As outlined above, amino acid substitutions are generally therefore based on the relative similarity of the amino acid side-chain substituents, for example, their hydrophobicity, hydrophilicity, charge, size, and the like. Exemplary substitutions that take various of the foregoing characteristics into consideration are well known to those of skill in the art and include: arginine and lysine; glutamate and aspartate; serine and threonine; glutamine and asparagine; and valine, leucine and isoleucine.

[0163] In addition, any polynucleotide may be further modified to increase stability in vivo. Possible modifications include, but are not limited to, the addition of flanking sequences at the 5′ and/or 3′ ends; the use of phosphorothioate or 2′ O-methyl rather than phosphodiesterase linkages in the backbone; and/or the inclusion of nontraditional bases such as inosine, queosine and wybutosine, as well as acetyl- methyl-, thio- and other modified forms of adenine, cytidine, guanine, thymine and uridine.

[0164] Amino acid substitutions may further be made on the basis of similarity in polarity, charge, solubility, hydrophobicity, hydrophilicity and/or the amphipathic nature of the residues. For example, negatively charged amino acids include aspartic acid and glutamic acid; positively charged amino acids include lysine and arginine; and amino acids with uncharged polar head groups having similar hydrophilicity values include leucine, isoleucine and valine; glycine and alanine; asparagine and glutamine; and serine, threonine, phenylalanine and tyrosine. Other groups of amino acids that may represent conservative changes include: (1) ala, pro, gly, glu, asp, gln, asn, ser, thr; (2) cys, ser, tyr, thr; (3) val, ile, leu, met, ala, phe; (4) lys, arg, his; and (5) phe, tyr, trp, his. A variant may also, or alternatively, contain nonconservative changes. In a preferred embodiment, variant polypeptides differ from a native sequence by substitution, deletion or addition of five amino acids or fewer. Variants may also (or alternatively) be modified by, for example, the deletion or addition of amino acids that have minimal influence on the immunogenicity, secondary structure and hydropathic nature of the polypeptide.

[0165] As noted above, polypeptides may comprise a signal (or leader) sequence at the N-terminal end of the protein, which co-translationally or post-translationally directs transfer of the protein. The polypeptide may also be conjugated to a linker or other sequence for ease of synthesis, purification or identification of the polypeptide (e.g., poly-His), or to enhance binding of the polypeptide to a solid support. For example, a polypeptide may be conjugated to an immunoglobulin Fc region.

[0166] When comparing polypeptide sequences, two sequences are said to be “identical” if the sequence of amino acids in the two sequences is the same when aligned for maximum correspondence, as described below. Comparisons between two sequences are typically performed by comparing the sequences over a comparison window to identify and compare local regions of sequence similarity. A “comparison window” as used herein, refers to a segment of at least about 20 contiguous positions, usually 30 to about 75, 40 to about 50, in which a sequence may be compared to a reference sequence of the same number of contiguous positions after the two sequences are optimally aligned.

[0167] Optimal alignment of sequences for comparison may be conducted using the Megalign program in the Lasergene suite of bioinformatics software (DNASTAR, Inc., Madison, Wis.), using default parameters. This program embodies several alignment schemes described in the following references: Dayhoff, M. O. (1978) A model of evolutionary change in proteins—Matrices for detecting distant relationships. In Dayhoff, M. O. (ed.) Atlas of Protein Sequence and Structure, National Biomedical Research Foundation, Washington D.C. Vol. 5, Suppl. 3, pp. 345-358; Hein J. (1990) Unified Approach to Alignment and Phylogenes pp. 626-645 Methods in Enzymology vol. 183, Academic Press, Inc., San Diego, Calif.; Higgins, D. G. and Sharp. P. M. (1989) CABIOS 5:151-153; Myers, E. W. and Muller W. (1988) CABIOS 4:11-17; Robinson, E. D. (1971) Comb. Theor. 11:105; Santou, N. Nes, M. (1987) Mol. Biol. Evol. 4:406-425; Sneath, P. H. A. and Sokal, R. R. (1973) Numerical Taxonomy—the Principles and Practice of Numerical Taxonomy, Freeman Press, San Francisco, Calif.; Wilbur, W. J. and Lipman, D. J. (1983) Proc. Natl. Acad., Sci. USA 80:726-730.

[0168] Alternatively, optimal alignment of sequences for comparison may be conducted by the local identity algorithm of Smith and Waterman (1981) Add. APL. Math 2:482, by the identity alignment algorithm of Needleman and Wunsch (1970) J. Mol. Biol. 48:443, by the search for similarity methods of Pearson and Lipman (1988) Proc. Natl. Acad. Sci. USA 85: 2444, by computerized implementations of these algorithms (GAP, BESTFIT, BLAST, FASTA, and TFASTA in the Wisconsin Genetics Software Package, Genetics Computer Group (GCG), 575 Science Dr., Madison, Wis.), or by inspection.

[0169] One preferred example of algorithms that are suitable for determining percent sequence identity and sequence similarity are the BLAST and BLAST 2.0 algorithms, which are described in Altschul et al. (1977) Nucl. Acids Res. 25:3389-3402 and Altschul et al. (1990) J. Mol. Biol. 215:403-410, respectively. BLAST and BLAST 2.0 can be used, for example with the parameters described herein, to determine percent sequence identity for the polynucleotides and polypeptides of the invention. Software for performing BLAST analyses is publicly available through the National Center for Biotechnology Information. For amino acid sequences, a scoring matrix can be used to calculate the cumulative score. Extension of the word hits in each direction are halted when: the cumulative alignment score falls off by the quantity X from its maximum achieved value; the cumulative score goes to zero or below, due to the accumulation of one or more negative-scoring residue alignments; or the end of either sequence is reached. The BLAST algorithm parameters W, T and X determine the sensitivity and speed of the alignment.

[0170] In one preferred approach, the “percentage of sequence identity” is determined by comparing two optimally aligned sequences over a window of comparison of at least 20 positions, wherein the portion of the polypeptide sequence in the comparison window may comprise additions or deletions (i.e., gaps) of 20 percent or less, usually 5 to 15 percent, or 10 to 12 percent, as compared to the reference sequences (which does not comprise additions or deletions) for optimal alignment of the two sequences. The percentage is calculated by determining the number of positions at which the identical amino acid residue occurs in both sequences to yield the number of matched positions, dividing the number of matched positions by the total number of positions in the reference sequence (i.e., the window size) and multiplying the results by 100 to yield the percentage of sequence identity.

[0171] Within other illustrative embodiments, a polypeptide may be a fusion polypeptide that comprises multiple polypeptides as described herein, or that comprises at least one polypeptide as described herein and an unrelated sequence, such as a known tumor protein. A fusion partner may, for example, assist in providing T helper epitopes (an immunological fusion partner), preferably T helper epitopes recognized by humans, or may assist in expressing the protein (an expression enhancer) at higher yields than the native recombinant protein. Certain preferred fusion partners are both immunological and expression enhancing fusion partners. Other fusion partners may be selected so as to increase the solubility of the polypeptide or to enable the polypeptide to be targeted to desired intracellular compartments. Still further fusion partners include affinity tags, which facilitate purification of the polypeptide.

[0172] Fusion polypeptides may generally be prepared using standard techniques, including chemical conjugation. Preferably, a fusion polypeptide is expressed as a recombinant polypeptide, allowing the production of increased levels, relative to a non-fused polypeptide, in an expression system. Briefly, DNA sequences encoding the polypeptide components may be assembled separately, and ligated into an appropriate expression vector. The 3′ end of the DNA sequence encoding one polypeptide component is ligated, with or without a peptide linker, to the 5′ end of a DNA sequence encoding the second polypeptide component so that the reading frames of the sequences are in phase. This permits translation into a single fusion polypeptide that retains the biological activity of both component polypeptides.

[0173] A peptide linker sequence may be employed to separate the first and second polypeptide components by a distance sufficient to ensure that each polypeptide folds into its secondary and tertiary structures. Such a peptide linker sequence is incorporated into the fusion polypeptide using standard techniques well known in the art. Suitable peptide linker sequences may be chosen based on the following factors: (1) their ability to adopt a flexible extended conformation; (2) their inability to adopt a secondary structure that could interact with functional epitopes on the first and second polypeptides; and (3) the lack of hydrophobic or charged residues that might react with the polypeptide functional epitopes. Preferred peptide linker sequences contain Gly, Asn and Ser residues. Other near neutral amino acids, such as Thr and Ala may also be used in the linker sequence. Amino acid sequences which may be usefully employed as linkers include those disclosed in Maratea et al., Gene 40:39-46, 1985; Murphy et al., Proc. Natl. Acad. Sci. USA 83:8258-8262, 1986; U.S. Pat. No. 4,935,233 and U.S. Pat. No. 4,751,180. The linker sequence may generally be from 1 to about 50 amino acids in length. Linker sequences are not required when the first and second polypeptides have non-essential N-terminal amino acid regions that can be used to separate the functional domains and prevent steric interference.

[0174] The ligated DNA sequences are operably linked to suitable transcriptional or translational regulatory elements. The regulatory elements responsible for expression of DNA are located only 5′ to the DNA sequence encoding the first polypeptides. Similarly, stop codons required to end translation and transcription termination signals are only present 3′ to the DNA sequence encoding the second polypeptide.

[0175] The fusion polypeptide can comprise a polypeptide as described herein together with an unrelated immunogenic protein, such as an immunogenic protein capable of eliciting a recall response. Examples of such proteins include tetanus, tuberculosis and hepatitis proteins (see, for example, Stoute et al. New Engl. J Med., 336:86-91, 1997).

[0176] In one preferred embodiment, the immunological fusion partner is derived from a Mycobacterium sp., such as a Mycobacterium tuberculosis-derived Ra12 fragment. Ra12 compositions and methods for their use in enhancing the expression and/or immunogenicity of heterologous polynucleotide/polypeptide sequences is described in U.S. patent application Ser. No. 60/158,585, the disclosure of which is incorporated herein by reference in its entirety. Briefly, Ra12 refers to a polynucleotide region that is a subsequence of a Mycobacterium tuberculosis MTB32A nucleic acid. MTB32A is a serine protease of 32 KD molecular weight encoded by a gene in virulent and avirulent strains of M. tuberculosis. The nucleotide sequence and amino acid sequence of MTB32A have been described (for example, U.S. patent application Ser. No. 60/158,585; see also, Skeiky et al, Infection and Immun. (1999) 67:3998-4007, incorporated herein by reference). C-terminal fragments of the MTB32A coding sequence express at high levels and remain as a soluble polypeptides throughout the purification process. Moreover, Ra12 may enhance the immunogenicity of heterologous immunogenic polypeptides with which it is fused. One preferred Ra12 fusion polypeptide comprises a 14 KD C-terminal fragment corresponding to amino acid residues 192 to 323 of MTB32A. Other preferred Ra12 polynucleotides generally comprise at least about 15 consecutive nucleotides, at least about 30 nucleotides, at least about 60 nucleotides, at least about 100 nucleotides, at least about 200 nucleotides, or at least about 300 nucleotides that encode a portion of a Ra12 polypeptide. Ra12 polynucleotides may comprise a native sequence (i.e., an endogenous sequence that encodes a Ra12 polypeptide or a portion thereof or may comprise a variant of such a sequence. Ra12 polynucleotide variants may contain one or more substitutions, additions, deletions and/or insertions such that the biological activity of the encoded fusion polypeptide is not substantially diminished, relative to a fusion polypeptide comprising a native Ra12 polypeptide. Variants preferably exhibit at least about 70% identity, more preferably at least about 80% identity and most preferably at least about 90% identity to a polynucleotide sequence that encodes a native Ra12 polypeptide or a portion thereof.

[0177] Within other preferred embodiments, an immunological fusion partner is derived from protein D, a surface protein of the gram-negative bacterium Haemophilus influenza B (WO 91/18926). Preferably, a protein D derivative comprises approximately the first third of the protein (e.g., the first N-terminal 100-110 amino acids), and a protein D derivative may be lipidated. Within certain preferred embodiments, the first 109 residues of a Lipoprotein D fusion partner is included on the N-terminus to provide the polypeptide with additional exogenous T-cell epitopes and to increase the expression level in E. coli (thus functioning as an expression enhancer). The lipid tail ensures optimal presentation of the antigen to antigen presenting cells. Other fusion partners include the non-structural protein from influenzae virus, NS1 (hemaglutinin). Typically, the N-terminal 81 amino acids are used, although different fragments that include T-helper epitopes may be used.

[0178] In another embodiment, the immunological fusion partner is the protein known as LYTA, or a portion thereof (preferably a C-terminal portion). LYTA is derived from Streptococcus pneumoniae, which synthesizes an N-acetyl-L-alanine amidase known as amidase LYTA (encoded by the LytA gene; Gene 43:265-292, 1986). LYTA is an autolysin that specifically degrades certain bonds in the peptidoglycan backbone. The C-terminal domain of the LYTA protein is responsible for the affinity to the choline or to some choline analogues such as DEAE. This property has been exploited for the development of E. coli C-LYTA expressing plasmids useful for expression of fusion proteins. Purification of hybrid proteins containing the C-LYTA fragment at the amino terminus has been described (see Biotechnology 10:795-798, 1992). Within a preferred embodiment, a repeat portion of LYTA may be incorporated into a fusion polypeptide. A repeat portion is found in the C-terminal region starting at residue 178. A particularly preferred repeat portion incorporates residues 188-305.

[0179] Yet another illustrative embodiment involves fusion polypeptides, and the polynucleotides encoding them, wherein the fusion partner comprises a targeting signal capable of directing a polypeptide to the endosomal/lysosomal compartment, as described in U.S. Pat. No. 5,633,234. An immunogenic polypeptide of the invention, when fused with this targeting signal, will associate more efficiently with MHC class II molecules and thereby provide enhanced in vivo stimulation of CD4⁺ T-cells specific for the polypeptide.

[0180] Polypeptides of the invention are prepared using any of a variety of well known synthetic and/or recombinant techniques, the lafter of which are further described below. Polypeptides, portions and other variants generally less than about 150 amino acids can be generated by synthetic means, using techniques well known to those of ordinary skill in the art. In one illustrative example, such polypeptides are synthesized using any of the commercially available solid-phase techniques, such as the Merrifield solid-phase synthesis method, where amino acids are sequentially added to a growing amino acid chain. See Merrifield, J. Am. Chem. Soc. 85:2149-2146,1963. Equipment for automated synthesis of polypeptides is commercially available from suppliers such as Perkin Elmer/Applied BioSystems Division (Foster City, Calif.), and may be operated according to the manufacturer's instructions.

[0181] In general, polypeptide compositions (including fusion polypeptides) of the invention are isolated. An “isolated” polypeptide is one that is removed from its original environment. For example, a naturally-occurring protein or polypeptide is isolated if it is separated from some or all of the coexisting materials in the natural system. Preferably, such polypeptides are also purified, e.g., are at least about 90% pure. more preferably at least about 95% pure and most preferably at least about 99% pure.

[0182] Polynucleotide Compositions

[0183] The present invention, in other aspects, provides polynucleotide compositions. The terms “DNA” and “polynucleotide” are used essentially interchangeably herein to refer to a DNA molecule that has been isolated free of total genomic DNA of a particular species. “Isolated,” as used herein, means that a polynucleotide is substantially away from other coding sequences, and that the DNA molecule does not contain large portions of unrelated coding DNA, such as large chromosomal fragments or other functional genes or polypeptide coding regions. Of course, this refers to the DNA molecule as originally isolated, and does not exclude genes or coding regions later added to the segment by the hand of man.

[0184] As will be understood by those skilled in the art, the polynucleotide compositions of this invention can include genomic sequences, extra-genomic and plasmid-encoded sequences and smaller engineered gene segments that express, or may be adapted to express, proteins, polypeptides, peptides and the like. Such segments may be naturally isolated, or modified synthetically by the hand of man.

[0185] As will be also recognized by the skilled artisan, polynucleotides of the invention may be single-stranded (coding or antisense) or double-stranded, and may be DNA (genomic, cDNA or synthetic) or RNA molecules. RNA molecules may include HnRNA molecules, which contain introns and correspond to a DNA molecule in a one-to-one manner, and mRNA molecules, which do not contain introns. Additional coding or non-coding sequences may, but need not, be present within a polynucleotide of the present invention, and a polynucleotide may, but need not, be linked to other molecules and/or support materials.

[0186] Polynucleotides may comprise a native sequence (i.e., an endogenous sequence that encodes a polypeptide/protein of the invention or a portion thereof or may comprise a sequence that encodes a variant or derivative. preferably and immunogenic variant or derivative, of such a sequence.

[0187] Therefore, according to another aspect of the present invention, polynucleotide compositions are provided that comprise some or all of a polynucleotide sequence set forth in any one of SEQ ID NO:1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288, complements of a polynucleotide sequence set forth as described above, and degenerate variants of a polynucleotide sequence set forth as described above. In certain preferred embodiments, the polynucleotide sequences set forth herein encode immunogenic polypeptides, as described above.

[0188] In other related embodiments, the present invention provides polynucleotide variants having substantial identity to the sequences disclosed herein in SEQ ID NO:1-185, 187-199, 203-206, 208, 210-214, 216-246, 250-256, 262-268, 273-277, 283, 285, and 287-288, for example those comprising at least 70% sequence identity, preferably at least 75%, 80%, 85%, 90%, 95%, 96%, 97%, 98%, or 99% or higher, sequence identity compared to a polynucleotide sequence of this invention using the methods described herein, (e.g., BLAST analysis using standard parameters, as described below). One skilled in this art will recognize that these values can be appropriately adjusted to determine corresponding identity of proteins encoded by two nucleotide sequences by taking into account codon degeneracy, amino acid similarity, reading frame positioning and the like.

[0189] Typically, polynucleotide variants will contain one or more substitutions, additions, deletions and/or insertions, preferably such that the immunogenicity of the polypeptide encoded by the variant polynucleotide is not substantially diminished relative to a polypeptide encoded by a polynucleotide sequence specifically set forth herein). The term “variants” should also be understood to encompasses homologous genes of xenogenic origin.

[0190] In additional embodiments, the present invention provides polynucleotide fragments comprising various lengths of contiguous stretches of sequence identical to or complementary to one or more of the sequences disclosed herein. For example, polynucleotides are provided by this invention that comprise at least about 10, 15, 20, 30, 40, 50, 75, 100,150, 200, 300, 400, 500 or 1000 or more contiguous nucleotides of one or more of the sequences disclosed herein as well as all intermediate lengths there between. It will be readily understood that “intermediate lengths”, in this context, means any length between the quoted values, such as 16, 17, 18, 19, etc.; 21, 22, 23, etc.; 30, 31, 32, etc.; 50, 51, 52, 53, etc.; 100, 101, 102, 103, etc.; 150, 151, 152, 153, etc.; including all integers through 200-500; 500-1,000, and the like.

[0191] In another embodiment of the invention, polynucleotide compositions are provided that are capable of hybridizing under moderate to high stringency conditions to a polynucleotide sequence provided herein, or a fragment thereof, or a complementary sequence thereof. Hybridization techniques are well known in the art of molecular biology. For purposes of illustration, suitable moderately stringent conditions for testing the hybridization of a polynucleotide of this invention with other polynucleotides include prewashing in a solution of 5×SSC, 0.5% SDS, 1.0 mM EDTA (pH 8.0); hybridizing at 50° C.-60° C., 5×SSC, overnight; followed by washing twice at 65° C. for 20 minutes with each of 2×, 0.5× and 0.2× SSC containing 0.1% SDS. One skilled in the art will understand that the stringency of hybridization can be readily manipulated, such as by altering the salt content of the hybridization solution and/or the temperature at which the hybridization is performed. For example, in another embodiment, suitable highly stringent hybridization conditions include those described above, with the exception that the temperature of hybridization is increased, e.g., to 60-65° C. or 65-70° C.

[0192] In certain preferred embodiments, the polynucleotides described above, e.g., polynucleotide variants, fragments and hybridizing sequences, encode polypeptides that are immunologically cross-reactive with a polypeptide sequence specifically set forth herein. In other preferred embodiments, such polynucleotides encode polypeptides that have a level of immunogenic activity of at least about 50%, preferably at least about 70%, and more preferably at least about 90% of that for a polypeptide sequence specifically set forth herein.

[0193] The polynucleotides of the present invention, or fragments thereof, regardless of the length of the coding sequence itself, may be combined with other DNA sequences, such as promoters, polyadenylation signals, additional restriction enzyme sites, multiple cloning sites, other coding segments, and the like, such that their overall length may vary considerably. It is therefore contemplated that a nucleic acid fragment of almost any length may be employed, with the total length preferably being limited by the ease of preparation and use in the intended recombinant DNA protocol. For example, illustrative polynucleotide segments with total lengths of about 10,000, about 5000, about 3000, about 2,000, about 1,000, about 500, about 200, about 100, about 50 base pairs in length, and the like, (including all intermediate lengths) are contemplated to be useful in many implementations of this invention.

[0194] When comparing polynucleotide sequences, two sequences are said to be “identical” if the sequence of nucleotides in the two sequences is the same when aligned for maximum correspondence, as described below. Comparisons between two sequences are typically performed by comparing the sequences over a comparison window to identify and compare local regions of sequence similarity. A “comparison window” as used herein, refers to a segment of at least about 20 contiguous positions, usually 30 to about 75, 40 to about 50, in which a sequence may be compared to a reference sequence of the same number of contiguous positions after the two sequences are optimally aligned.

[0195] Optimal alignment of sequences for comparison may be conducted using the Megalign program in the Lasergene suite of bioinformatics software (DNASTAR, Inc., Madison, Wis.), using default parameters. This program embodies several alignment schemes described in the following references: Dayhoff, M. O. (1978) A model of evolutionary change in proteins—Matrices for detecting distant relationships. In Dayhoff. M. O. (ed.) Atlas of Protein Sequence and Structure, National Biomedical Research Foundation, Washington D.C. Vol. 5, Suppl. 3, pp. 345-358; Hein J. (1990) Unified Approach to Alignment and Phylogenes pp. 626-645 Methods in Enzymology vol. 183, Academic Press, Inc., San Diego, Calif.; Higgins, D. G. and Sharp, P. M. (1989) CABIOS 5:151-153; Myers, E. W. and Muller W. (1988) CABIOS 4:11-17; Robinson, E. D. (1971) Comb. Theor 11:105; Santou, N. Nes, M. (1987) Mol. Biol. Evol. 4:406-425; Sneath, P. H. A. and Sokal, R. R. (1973) Numerical Taxonomy—the Principles and Practice of Numerical Taxonomy, Freeman Press, San Francisco, Calif.; Wilbur, W. J. and Lipman, D. J. (1983) Proc. Natl. Acad., Sci. USA 80:726-730.

[0196] Alternatively, optimal alignment of sequences for comparison may be conducted by the local identity algorithm of Smith and Waterman (1981) Add. APL. Math 2:482, by the identity alignment algorithm of Needleman and Wunsch (1970) J. Mol. Biol. 48:443, by the search for similarity methods of Pearson and Lipman (1988) Proc. Natl. Acad. Sci. USA 85: 2444, by computerized implementations of these algorithms (GAP, BESTFIT, BLAST, FASTA, and TFASTA in the Wisconsin Genetics Software Package, Genetics Computer Group (GCG), 575 Science Dr., Madison, Wis.), or by inspection.

[0197] One preferred example of algorithms that are suitable for determining percent sequence identity and sequence similarity are the BLAST and BLAST 2.0 algorithms, which are described in Altschul et al. (1977) Nucl. Acids Res. 25:3389-3402 and Altschul et al. (1990) J. Mol. Biol. 215:403-410, respectively. BLAST and BLAST 2.0 can be used, for example with the parameters described herein, to determine percent sequence identity for the polynucleotides of the invention. Software for performing BLAST analyses is publicly available through the National Center for Biotechnology Information. In one illustrative example, cumulative scores can be calculated using, for nucleotide sequences, the parameters M (reward score for a pair of matching residues; always>0) and N (penalty score for mismatching residues; always<0). Extension of the word hits in each direction are halted when: the cumulative alignment score falls off by the quantity X from its maximum achieved value; the cumulative score goes to zero or below, due to the accumulation of one or more negative-scoring residue alignments; or the end of either sequence is reached. The BLAST algorithm parameters W, T and X determine the sensitivity and speed of the alignment. The BLASTN program (for nucleotide sequences) uses as defaults a wordlength (W) of 11, and expectation (E) of 10, and the BLOSUM62 scoring matrix (see Henikoff and Henikoff (1989) Proc. Natl. Acad. Sci. USA 89:10915) alignments, (B) of 50, expectation (E) of 10, M=5, N=−4 and a comparison of both strands.

[0198] Preferably, the “percentage of sequence identity” is determined by comparing two optimally aligned sequences over a window of comparison of at least 20 positions, wherein the portion of the polynucleotide sequence in the comparison window may comprise additions or deletions (i.e., gaps) of 20 percent or less, usually 5 to 15 percent, or 10 to 12 percent, as compared to the reference sequences (which does not comprise additions or deletions) for optimal alignment of the two sequences. The percentage is calculated by determining the number of positions at which the identical nucleic acid bases occurs in both sequences to yield the number of matched positions, dividing the number of matched positions by the total number of positions in the reference sequence (i.e., the window size) and multiplying the results by 100 to yield the percentage of sequence identity.

[0199] It will be appreciated by those of ordinary skill in the art that, as a result of the degeneracy of the genetic code, there are many nucleotide sequences that encode a polypeptide as described herein. Some of these polynucleotides bear minimal homology to the nucleotide sequence of any native gene. Nonetheless, polynucleotides that vary due to differences in codon usage are specifically contemplated by the present invention. Further, alleles of the genes comprising the polynucleotide sequences provided herein are within the scope of the present invention. Alleles are endogenous genes that are altered as a result of one or more mutations, such as deletions, additions and/or substitutions of nucleotides. The resulting mRNA and protein may, but need not, have an altered structure or function. Alleles may be identified using standard techniques (such as hybridization, amplification and/or database sequence comparison).

[0200] Therefore, in another embodiment of the invention, a mutagenesis approach, such as site-specific mutagenesis, is employed for the preparation of immunogenic variants and/or derivatives of the polypeptides described herein. By this approach, specific modifications in a polypeptide sequence can be made through mutagenesis of the underlying polynucleotides that encode them. These techniques provides a straightforward approach to prepare and test sequence variants, for example, incorporating one or more of the foregoing considerations, by introducing one or more nucleotide sequence changes into the polynucleotide.

[0201] Site-specific mutagenesis allows the production of mutants through the use of specific oligonucleotide sequences which encode the DNA sequence of the desired mutation, as well as a sufficient number of adjacent nucleotides, to provide a primer sequence of sufficient size and sequence complexity to form a stable duplex on both sides of the deletion junction being traversed. Mutations may be employed in a selected polynucleotide sequence to improve, alter, decrease, modify, or otherwise change the properties of the polynucleotide itself, and/or alter the properties, activity, composition, stability, or primary sequence of the encoded polypeptide.

[0202] In certain embodiments of the present invention, the inventors contemplate the mutagenesis of the disclosed polynucleotide sequences to alter one or more properties of the encoded polypeptide, such as the immunogenicity of a polypeptide vaccine. The techniques of site-specific mutagenesis are well-known in the art, and are widely used to create variants of both polypeptides and polynucleotides. For example, site-specific mutagenesis is often used to alter a specific portion of a DNA molecule. In such embodiments, a primer comprising typically about 14 to about 25 nucleotides or so in length is employed, with about 5 to about 10 residues on both sides of the junction of the sequence being altered.

[0203] As will be appreciated by those of skill in the art, site-specific mutagenesis techniques have often employed a phage vector that exists in both a single stranded and double stranded form. Typical vectors useful in site-directed mutagenesis include vectors such as the M13 phage. These phage are readily commercially-available and their use is generally well-known to those skilled in the art. Double-stranded plasmids are also routinely employed in site directed mutagenesis that eliminates the step of transferring the gene of interest from a plasmid to a phage.

[0204] In general, site-directed mutagenesis in accordance herewith is performed by first obtaining a single-stranded vector or melting apart of two strands of a double-stranded vector that includes within its sequence a DNA sequence that encodes the desired peptide. An oligonucleotide primer bearing the desired mutated sequence is prepared, generally synthetically. This primer is then annealed with the single-stranded vector, and subjected to DNA polymerizing enzymes such as E. coli polymerase I Klenow fragment, in order to complete the synthesis of the mutation-bearing strand. Thus, a heteroduplex is formed wherein one strand encodes the original non-mutated sequence and the second strand bears the desired mutation. This heteroduplex vector is then used to transform appropriate cells, such as E. coli cells, and clones are selected which include recombinant vectors bearing the mutated sequence arrangement.

[0205] The preparation of sequence variants of the selected peptide-encoding DNA segments using site-directed mutagenesis provides a means of producing potentially useful species and is not meant to be limiting as there are other ways in which sequence variants of peptides and the DNA sequences encoding them may be obtained. For example, recombinant vectors encoding the desired peptide sequence may be treated with mutagenic agents, such as hydroxylamine, to obtain sequence variants. Specific details regarding these methods and protocols are found in the teachings of Maloy et al., 1994; Segal, 1976; Prokop and Bajpai, 1991: Kuby, 1994: and Maniatis et al., 1982. each incorporated herein by reference, for that purpose.

[0206] As used herein, the term “oligonucleotide directed mutagenesis procedure” refers to template-dependent processes and vector-mediated propagation which result in an increase in the concentration of a specific nucleic acid molecule relative to its initial concentration, or in an increase in the concentration of a detectable signal, such as amplification. As used herein, the term “oligonucleotide directed mutagenesis procedure” is intended to refer to a process that involves the template-dependent extension of a primer molecule. The term template dependent process refers to nucleic acid synthesis of an RNA or a DNA molecule wherein the sequence of the newly synthesized strand of nucleic acid is dictated by the well-known rules of complementary base pairing (see, for example, Watson, 1987). Typically, vector mediated methodologies involve the introduction of the nucleic acid fragment into a DNA or RNA vector, the clonal amplification of the vector, and the recovery of the amplified nucleic acid fragment. Examples of such methodologies are provided by U.S. Pat. No. 4,237,224, specifically incorporated herein by reference in its entirety.

[0207] In another approach for the production of polypeptide variants of the present invention, recursive sequence recombination, as described in U.S. Pat. No. 5,837,458, may be employed. In this approach, iterative cycles of recombination and screening or selection are performed to “evolve” individual polynucleotide variants of the invention having, for example, enhanced immunogenic activity.

[0208] In other embodiments of the present invention, the polynucleotide sequences provided herein can be advantageously used as probes or primers for nucleic acid hybridization. As such, it is contemplated that nucleic acid segments that comprise a sequence region of at least about 15 nucleotide long contiguous sequence that has the same sequence as, or is complementary to, a 15 nucleotide long contiguous sequence disclosed herein will find particular utility. Longer contiguous identical or complementary sequences. e.g., those of about 20, 30, 40, 50, 100, 200, 500, 1000 (including all intermediate lengths) and even up to full length sequences will also be of use in certain embodiments.

[0209] The ability of such nucleic acid probes to specifically hybridize to a sequence of interest will enable them to be of use in detecting the presence of complementary sequences in a given sample. However, other uses are also envisioned, such as the use of the sequence information for the preparation of mutant species primers, or primers for use in preparing other genetic constructions.

[0210] Polynucleotide molecules having sequence regions consisting of contiguous nucleotide stretches of 10-14, 15-20, 30, 50, or even of 100-200 nucleotides or so (including intermediate lengths as well), identical or complementary to a polynucleotide sequence disclosed herein, are particularly contemplated as hybridization probes for use in, e.g., Southern and Northern blotting. This would allow a gene product, or fragment thereof, to be analyzed, both in diverse cell types and also in various bacterial cells. The total size of fragment, as well as the size of the complementary stretch(es), will ultimately depend on the intended use or application of the particular nucleic acid segment. Smaller fragments will generally find use in hybridization embodiments, wherein the length of the contiguous complementary region may be varied, such as between about 15 and about 100 nucleotides, but larger contiguous complementarity stretches may be used, according to the length complementary sequences one wishes to detect.

[0211] The use of a hybridization probe of about 15-25 nucleotides in length allows the formation of a duplex molecule that is both stable and selective. Molecules having contiguous complementary sequences over stretches greater than 15 bases in length are generally preferred, though, in order to increase stability and selectivity of the hybrid, and thereby improve the quality and degree of specific hybrid molecules obtained. One will generally prefer to design nucleic acid molecules having gene-complementary stretches of 15 to 25 contiguous nucleotides, or even longer where desired.

[0212] Hybridization probes may be selected from any portion of any of the sequences disclosed herein. All that is required is to review the sequences set forth herein, or to any continuous portion of the sequences, from about 15-25 nucleotides in length up to and including the full length sequence, that one wishes to utilize as a probe or primer. The choice of probe and primer sequences may be governed by various factors. For example, one may wish to employ primers from towards the termini of the total sequence.

[0213] Small polynucleotide segments or fragments may be readily prepared by, for example, directly synthesizing the fragment by chemical means, as is commonly practiced using an automated oligonucleotide synthesizer. Also, fragments may be obtained by application of nucleic acid reproduction technology, such as the PCR™ technology of U.S. Pat. No. 4,683,202 (incorporated herein by reference), by introducing selected sequences into recombinant vectors for recombinant production, and by other recombinant DNA techniques generally known to those of skill in the art of molecular biology.

[0214] The nucleotide sequences of the invention may be used for their ability to selectively form duplex molecules with complementary stretches of the entire gene or gene fragments of interest. Depending on the application envisioned, one will typically desire to employ varying conditions of hybridization to achieve varying degrees of selectivity of probe towards target sequence. For applications requiring high selectivity, one will typically. desire to employ relatively stringent conditions to form the hybrids, e.g., one will select relatively low salt and/or high temperature conditions, such as provided by a salt concentration of from about 0.02 M to about 0.15 M salt at temperatures of from about 50° C. to about 70° C. Such selective conditions tolerate little, if any, mismatch between the probe and the template or target strand, and would be particularly suitable for isolating related sequences.

[0215] Of course, for some applications, for example, where one desires to prepare mutants employing a mutant primer strand hybridized to an underlying template, less stringent (reduced stringency) hybridization conditions will typically be needed in order to allow formation of the heteroduplex. In these circumstances, one may desire to employ salt conditions such as those of from about 0.15 M to about 0.9 M salt, at temperatures ranging from about 20° C. to about 55° C. Cross-hybridizing species can thereby be readily identified as positively hybridizing signals with respect to control hybridizations. In any case, it is generally appreciated that conditions can be rendered more stringent by the addition of increasing amounts of formamide, which serves to destabilize the hybrid duplex in the same manner as increased temperature. Thus, hybridization conditions can be readily manipulated, and thus will generally be a method of choice depending on the desired results.

[0216] According to another embodiment of the present invention, polynucleotide compositions comprising antisense oligonucleotides are provided. Antisense oligonucleotides have been demonstrated to be effective and targeted inhibitors of protein synthesis, and, consequently, provide a therapeutic approach by which a disease can be treated by inhibiting the synthesis of proteins that contribute to the disease. The efficacy of antisense oligonucleotides for inhibiting protein synthesis is well established. For example, the synthesis of polygalactauronase and the muscarine type 2 acetylcholine receptor are inhibited by antisense oligonucleotides directed to their respective mRNA sequences (U.S. Pat. No. 5,739,119 and U.S. Pat. No. 5,759,829). Further, examples of antisense inhibition have been demonstrated with the nuclear protein cyclin, the multiple drug resistance gene (MDG1), ICAM-1, E-selectin, STK-1, striatal GABA_(A) receptor and human EGF (Jaskulski et al., Science. Jun. 10, 1988; 240(4858):1544-6; Vasanthakumar and Ahmed, Cancer Commun. 1989; 1(4):225-32; Peris et al., Brain Res Mol Brain Res. Jun. 15, 1998; 57(2):310-20; U.S. Pat. No. 5,801,154; U.S. Pat. No. 5,789,573; U.S. Pat. No. 5,718,709 and U.S. Pat. No. 5,610,288). Antisense constructs have also been described that inhibit and can be used to treat a variety of abnormal cellular proliferations, e.g., cancer (U.S. Pat. No. 5,747,470; U.S. Pat. No. 5,591,317 and U.S. Pat. No. 5,783,683).

[0217] Therefore, in certain embodiments, the present invention provides oligonucleotide sequences that comprise all, or a portion of, any sequence that is capable of specifically binding to polynucleotide sequence described herein, or a complement thereof. In one embodiment, the antisense oligonucleotides comprise DNA or derivatives thereof. In another embodiment, the oligonucleotides comprise RNA or derivatives thereof. In a third embodiment, the oligonucleotides are modified DNAs comprising a phosphorothioated modified backbone. In a fourth embodiment, the oligonucleotide sequences comprise peptide nucleic acids or derivatives thereof. In each case, preferred compositions comprise a sequence region that is complementary, and more preferably substantially-complementary, and even more preferably, completely complementary to one or more portions of polynucleotides disclosed herein. Selection of antisense compositions specific for a given gene sequence is based upon analysis of the chosen target sequence and determination of secondary structure, T_(m), binding energy, and relative stability. Antisense compositions may be selected based upon their relative inability to form dimers, hairpins, or other secondary structures that would reduce or prohibit specific binding to the target mRNA in a host cell. Highly preferred target regions of the mRNA, are those which are at or near the AUG translation initiation codon, and those sequences which are substantially complementary to 5′ regions of the mRNA. These secondary structure analyses and target site selection considerations can be performed, for example, using v.4 of the OLIGO primer analysis software and/or the BLASTN 2.0.5 algorithm software (Altschul et al., Nucleic Acids Res. 1997, 25(17):3389-402).

[0218] The use of an antisense delivery method employing a short peptide vector, termed MPG (27 residues), is also contemplated. The MPG peptide contains a hydrophobic domain derived from the fusion sequence of HIV gp41 and a hydrophilic domain from the nuclear localization sequence of SV40 T-antigen (Morris et al., Nucleic Acids Res. Jul. 15, 1997; 25(14):2730-6). It has been demonstrated that several molecules of the MPG peptide coat the antisense oligonucleotides and can be delivered into cultured mammalian cells in less than 1 hour with relatively high efficiency (90%). Further, the interaction with MPG strongly increases both the stability of the oligonucleotide to nuclease and the ability to cross the plasma membrane.

[0219] According to another embodiment of the invention, the polynucleotide compositions described herein are used in the design and preparation of ribozyme molecules for inhibiting expression of the tumor polypeptides and proteins of the present invention in tumor cells. Ribozymes are RNA-protein complexes that cleave nucleic acids in a site-specific fashion. Ribozymes have specific catalytic domains that possess endonuclease activity (Kim and Cech, Proc Natl Acad Sci U S A. 1987 December; 84(24):8788-92; Forster and Symons, Cell. Apr. 24, 1987; 49(2):211-20). For example, a large number of ribozymes accelerate phosphoester transfer reactions with a high degree of specificity, often cleaving only one of several phosphoesters in an oligonucleotide substrate (Cech et al., Cell. 1981 December; 27(3 Pt 2):487-96; Michel and Westhof, J Mol Biol. Dec. 5, 1990; 216(3):585-610; Reinhold-Hurek and Shub, Nature. May 14, 1992; 357(6374):173-6). This specificity has been attributed to the requirement that the substrate bind via specific base-pairing interactions to the internal guide sequence (“IGS”) of the ribozyme prior to chemical reaction.

[0220] Six basic varieties of naturally-occurring enzymatic RNAs are known presently. Each can catalyze the hydrolysis of RNA phosphodiester bonds in trans (and thus can cleave other RNA molecules) under physiological conditions. In general, enzymatic nucleic acids act by first binding to a target RNA. Such binding occurs through the target binding portion of a enzymatic nucleic acid which is held in close proximity to an enzymatic portion of the molecule that acts to cleave the target RNA. Thus; the enzymatic nucleic acid first recognizes and then binds a target RNA through complementary base-pairing, and once bound to the correct site, acts enzymatically to cut the target RNA. Strategic cleavage of such a target RNA will destroy its ability to direct synthesis of an encoded protein. After an enzymatic nucleic acid has bound and cleaved its RNA target, it is released from that RNA to search for another target and can repeatedly bind and cleave new targets.

[0221] The enzymatic nature of a ribozyme is advantageous over many technologies, such as antisense technology (where a nucleic acid molecule simply binds to a nucleic acid target to block its translation) since the concentration of ribozyme necessary to affect a therapeutic treatment is lower than that of an antisense oligonucleotide. This advantage reflects the ability of the ribozyme to act enzymatically. Thus, a single ribozyme molecule is able to cleave many molecules of target RNA. In addition, the ribozyme is a highly specific inhibitor, with the specificity of inhibition depending not only on the base pairing mechanism of binding to the target RNA, but also on the mechanism of target RNA cleavage. Single mismatches, or base-substitutions, near the site of cleavage can completely eliminate catalytic activity of a ribozyme. Similar mismatches in antisense molecules do not prevent their action (Woolf et al., Proc Natl Acad Sci USA. Aug. 15, 1992; 89(16):7305-9). Thus, the specificity of action of a ribozyme is greater than that of an antisense oligonucleotide binding the same RNA site.

[0222] The enzymatic nucleic acid molecule may be formed in a hammerhead, hairpin, a hepatitis δ virus, group I intron or RNaseP RNA (in association with an RNA guide sequence) or Neurospora VS RNA motif. Examples of hammerhead motifs are described by Rossi et al., Nucleic Acids Res. Sep. 11, 1992; 20(17):4559-65. Examples of hairpin motifs are described by Hampel et al., (Eur. Pat. Appl. Publ. No. EP 0360257), Hampel and Tritz, Biochemistry Jun. 13, 1989; 28(12):4929-33; Hampel et al., Nucleic Acids Res. Jan. 25, 1990; 18(2):299-304 and U.S. Pat. No. 5,631,359. An example of the hepatitis δ virus motif is described by Perrotta and Been. Biochemistry. Dec. 1, 1992; 31(47):11843-52; an example of the RNaseP motif is described by Guerrier-Takada et al., Cell. December 1983; 35(3 Pt 2):849-57; Neurospora VS RNA ribozyme motif is described by Collins (Saville and Collins, Cell. May 18, 1990; 61(4):685-96; Saville and Collins, Proc Natl Acad Sci USA. Oct. 1, 1991; 88(19):8826-30; Collins and Olive, Biochemistry. Mar. 23, 1993; 32(11):2795-9); and an example of the Group I intron is described in (U.S. Pat. No. 4,987,071). All that is important in an enzymatic nucleic acid molecule of this invention is that it has a specific substrate binding site which is complementary to one or more of the target gene RNA regions, and that it have nucleotide sequences within or surrounding that substrate binding site which impart an RNA cleaving activity to the molecule. Thus the ribozyme constructs need not be limited to specific motifs mentioned herein.

[0223] Ribozymes may be designed as described in Int. Pat. Appl. Publ. No. WO 93/23569 and Int. Pat. Appl. Publ. No. WO 94/02595, each specifically incorporated herein by reference) and synthesized to be tested in vitro and in vivo, as described. Such ribozymes can also be optimized for delivery. While specific examples are provided, those in the art will recognize that equivalent RNA targets in other species can be utilized when necessary.

[0224] Ribozyme activity can be optimized by altering the length of the ribozyme binding arms, or chemically synthesizing ribozymes with modifications that prevent their degradation by serum ribonucleases (see, e.g., Int. Pat. Appl. Publ. No. WO 92/07065; Int. Pat. Appl. Publ. No. WO 93/15187; Int. Pat. Appl. Publ. No. WO 91/03162; Eur. Pat. Appl. Publ. No. 92110298.4; U.S. Pat. No. 5,334,711; and Int. Pat. Appl. Publ. No. WO 94/13688, which describe various chemical modifications that can be made to the sugar moieties of enzymatic RNA molecules), modifications which enhance their efficacy in cells, and removal of stem II bases to shorten RNA synthesis times and reduce chemical requirements.

[0225] Sullivan et al. (Int. Pat. Appl. Publ. No. WO 94/02595) describes the general methods for delivery of enzymatic RNA molecules. Ribozymes may be administered to cells by a variety of methods known to those familiar to the art; including, but not restricted to, encapsulation in liposomes, by iontophoresis, or by incorporation into other vehicles, such as hydrogels, cyclodextrins, biodegradable nanocapsules, and bioadhesive microspheres. For some indications, ribozymes may be directly delivered ex vivo to cells or tissues with or without the aforementioned vehicles. Alternatively, the RNA/vehicle combination may be locally delivered by direct inhalation, by direct injection or by use of a catheter, infusion pump or stent. Other routes of delivery include, but are not limited to, intravascular, intramuscular, subcutaneous or joint injection, aerosol inhalation, oral (tablet or pill form), topical, systemic, ocular, intraperitoneal and/or intrathecal delivery. More detailed descriptions of ribozyme delivery and administration are provided in Int. Pat. Appl. Publ. No. WO 94/02595 and Int. Pat. Appl. Publ. No. WO 93/23569, each specifically incorporated herein by reference.

[0226] Another means of accumulating high concentrations of a ribozyme(s) within cells is to incorporate the ribozyme-encoding sequences into a DNA expression vector. Transcription of the ribozyme sequences are driven from a promoter for eukaryotic RNA polymerase I (pol I), RNA polymerase II (pol II), or RNA polymerase III (pol III). Transcripts from pol II or pol III promoters will be expressed at high levels in all cells; the levels of a given pol II promoter in a given cell type will depend on the nature of the gene regulatory sequences (enhancers, silencers, etc.) present nearby. Prokaryotic RNA polymerase promoters may also be used, providing that the prokaryotic RNA polymerase enzyme is expressed in the appropriate cells Ribozymes expressed from such promoters have been shown to function in mammalian cells. Such transcription units can be incorporated into a variety of vectors for introduction into mammalian cells, including but not restricted to, plasmid DNA vectors, viral DNA vectors (such as adenovirus or adeno-associated vectors), or viral RNA vectors (such as retroviral, semliki forest virus, sindbis virus vectors).

[0227] In another embodiment of the invention. peptide nucleic acids (PNAs) compositions are provided. PNA is a DNA mimic in which the nucleobases are attached to a pseudopeptide backbone (Good and Nielsen, Antisense Nucleic Acid Drug Dev. 1997 7(4) 431-37). PNA is able to be utilized in a number methods that traditionally have used RNA or DNA. Often PNA sequences perform better in techniques than the corresponding RNA or DNA sequences and have utilities that are not inherent to RNA or DNA. A review of PNA including methods of making, characteristics of, and methods of using, is provided by Corey (Trends Biotechnol June 1997; 15(6):224-9). As such, in certain embodiments, one may prepare PNA sequences that are complementary to one or more portions of the ACE mRNA sequence, and such PNA compositions may be used to regulate, alter, decrease, or reduce the translation of ACE-specific mRNA, and thereby alter the level of ACE activity in a host cell to which such PNA compositions have been administered.

[0228] PNAs have 2-aminoethyl-glycine linkages replacing the normal phosphodiester backbone of DNA (Nielsen et al., Science Dec. 6, 1991; 254(5037):1497-500; Hanvey et al., Science. Nov. 27, 1992; 258(5087): 1481-5; Hyrup and Nielsen, Bioorg Med Chem. January 1996; 4(1):5-23). This chemistry has three important consequences: firstly, in contrast to DNA or phosphorothioate oligonucleotides, PNAs are neutral molecules; secondly, PNAs are achiral, which avoids the need to develop a stereoselective synthesis; and thirdly, PNA synthesis uses standard Boc or Fmoc protocols for solid-phase peptide synthesis, although other methods, including a modified Merrifield method, have been used.

[0229] PNA monomers or ready-made oligomers are commercially available from PerSeptive Biosystems (Framingham, Mass.). PNA syntheses by either Boc or Fmoc protocols are straightforward using manual or automated protocols (Norton et al., Bioorg Med Chem. April 1995; 3(4):437-45). The manual protocol lends itself to the production of chemically modified PNAs or the simultaneous synthesis of families of closely related PNAs.

[0230] As with peptide synthesis, the success of a particular PNA synthesis will depend on the properties of the chosen sequence. For example, while in theory PNAs can incorporate any combination of nucleotide bases, the presence of adjacent purines can lead to deletions of one or more residues in the product. In expectation of this difficulty, it is suggested that, in producing PNAs with adjacent purines, one should repeat the coupling of residues likely to be added inefficiently. This should be followed by the purification of PNAs by reverse-phase high-pressure liquid chromatography, providing yields and purity of product similar to those observed during the synthesis of peptides.

[0231] Modifications of PNAs for a given application may be accomplished by coupling amino acids during solid-phase synthesis or by attaching compounds that contain a carboxylic acid group to the exposed N-terminal amine. Alternatively, PNAs can be modified after synthesis by coupling to an introduced lysine or cysteine. The ease with which PNAs can be modified facilitates optimization for better solubility or for specific functional requirements. Once synthesized, the identity of PNAs and their derivatives can be confirmed by mass spectrometry. Several studies have made and utilized modifications of PNAs (for example, Norton et al., Bioorg Med Chem. April 1995; 3(4):437-45; Petersen et al., J Pept Sci. May-June 1995; 1(3):175-83; Orum et al., Biotechniques. September 1995; 19(3):472-80; Footer et al., Biochemistry. Aug. 20, 1996; 35(33):10673-9; Griffith et al., Nucleic Acids Res. Aug. 11, 1995; 23(15):3003-8; Pardridge et al., Proc Natl Acad Sci USA. Jun. 6, 1995; 92(12):5592-6; Boffa et al., Proc Natl Acad Sci USA. Mar. 14, 1995; 92(6):1901-5; Gambacorti-Passerini et al., Blood. Aug. 15, 1996; 88(4):1411-7; Armitage et al., Proc Natl Acad Sci USA. Nov. 11, 1997; 94(23):12320-5; Seeger et al., Biotechniques. September 1997; 23(3):512-7). U.S. Pat. No. 5,700,922 discusses PNA-DNA-PNA chimeric molecules and their uses in diagnostics, modulating protein in organisms, and treatment of conditions susceptible to therapeutics.

[0232] Methods of characterizing the antisense binding properties of PNAs are discussed in Rose (Anal Chem. Dec. 15, 1993; 65(24):3545-9) and Jensen et a. (Biochemistry. Apr. 22, 1997; 36(16):5072-7). Rose uses capillary gel electrophoresis to determine binding of PNAs to their complementary oligonucleotide, measuring the relative binding kinetics and stoichiometry. Similar types of measurements were made by Jensen et al. using BIAcore™ technology.

[0233] Other applications of PNAs that have been described and will be apparent to the skilled artisan include use in DNA strand invasion, antisense inhibition, mutational analysis, enhancers of transcription, nucleic acid purification, isolation of transcriptionally active genes, blocking of transcription factor binding, genome cleavage, biosensors, in situ hybridization, and the like.

[0234] Polynucleotide Identification, Characterization and Expression

[0235] Polynucleotides compositions of the present invention may be identified, prepared and/or manipulated using any of a variety of well established techniques (see generally, Sambrook et al., Molecular Cloning: A Laboratory Manual, Cold Spring Harbor Laboratories, Cold Spring Harbor, N.Y., 1989, and other like references). For example, a polynucleotide may be identified, as described in more detail below, by screening a microarray of cDNAs for tumor-associated expression (i.e., expression that is at least two fold greater in a tumor than in normal tissue, as determined using a representative assay provided herein). Such screens may be performed, for example, using the microarray technology of Affymetrix, Inc. (Santa Clara, Calif.) according to the manufacturer's instructions (and essentially as described by Schena et al., Proc. Natl. Acad. Sci. USA 93:10614-10619, 1996 and Heller et al., Proc. Natl. Acad. Sci. USA 94:2150-2155, 1997). Alternatively, polynucleotides may be amplified from cDNA prepared from cells expressing the proteins described herein, such as tumor cells.

[0236] Many template dependent processes are available to amplify a target sequences of interest present in a sample. One of the best known amplification methods is the polymerase chain reaction (PCR™) which is described in detail in U.S. Pat. Nos. 4,683,195, 4,683,202 and 4,800,159, each of which is incorporated herein by reference in its entirety. Briefly, in PCR™, two primer sequences are prepared which are complementary to regions on opposite complementary strands of the target sequence. An excess of deoxynucleoside triphosphates is added to a reaction mixture along with a DNA polymerase (e.g., Taq polymerase). If the target sequence is present in a sample, the primers will bind to the target and the polymerase will cause the primers to be extended along the target sequence by adding on nucleotides. By raising and lowering the temperature of the reaction mixture, the extended primers will dissociate from the target to form reaction products, excess primers will bind to the target and to the reaction product and the process is repeated. Preferably reverse transcription and PCR™ amplification procedure may be performed in order to quantify the amount of mRNA amplified. Polymerase chain reaction methodologies are well known in the art.

[0237] Any of a number of other template dependent processes, many of which are variations of the PCR™ amplification technique, are readily known and available in the art. Illustratively, some such methods include the ligase chain reaction (referred to as LCR), described, for example, in Eur. Pat. Appl. Publ. No. 320,308 and U.S. Pat. No. 4,883,750; Qbeta Replicase, described in PCT Intl. Pat. Appl. Publ. No. PCT/US87/00880; Strand Displacement Amplification (SDA) and Repair Chain Reaction (RCR). Still other amplification methods are described in Great Britain Pat. Appl. No. 2 202 328, and in PCT Intl. Pat. Appl. Publ. No. PCT/US89/01025. Other nucleic acid amplification procedures include transcription-based amplification systems (TAS) (PCT Intl. Pat. Appl. Publ. No. WO 88/10315), including nucleic acid sequence based amplification (NASBA) and 3SR. Eur. Pat. Appl. Publ. No. 329,822 describes a nucleic acid amplification process involving cyclically synthesizing single-stranded RNA (“ssRNA”), ssDNA, and double-stranded DNA (dsDNA). PCT Intl. Pat. Appl. Publ. No. WO 89/06700 describes a nucleic acid sequence amplification scheme based on the hybridization of a promoter/primer sequence to a target single-stranded DNA (“ssDNA”) followed by transcription of many RNA copies of the sequence. Other amplification methods such as “RACE” (Frohman, 1990), and “one-sided PCR” (Ohara, 1989) are also well-known to those of skill in the art.

[0238] An amplified portion of a polynucleotide of the present invention may be used to isolate a full length gene from a suitable library (e.g., a tumor cDNA library) using well known techniques. Within such techniques, a library (cDNA or genomic) is screened using one or more polynucleotide probes or primers suitable for amplification. Preferably, a library is size-selected to include larger molecules. Random primed libraries may also be preferred for identifying 5′ and upstream regions of genes. Genomic libraries are preferred for obtaining introns and extending 5′ sequences.

[0239] For hybridization techniques, a partial sequence may be labeled (e.g., by nick-translation or end-labeling with ³²P) using well known techniques. A bacterial or bacteriophage library is then generally screened by hybridizing filters containing denatured bacterial colonies (or lawns containing phage plaques) with the labeled probe (see Sambrook et al., Molecular Cloning: A Laboratory Manual, Cold Spring Harbor Laboratories, Cold Spring Harbor, N.Y., 1989). Hybridizing colonies or plaques are selected and expanded, and the DNA is isolated for further analysis. cDNA clones may be analyzed to determine the amount of additional sequence by, for example, PCR using a primer from the partial sequence and a primer from the vector. Restriction maps and partial sequences may be generated to identify one or more overlapping clones. The complete sequence may then be determined using standard techniques, which may involve generating a series of deletion clones. The resulting overlapping sequences can then assembled into a single contiguous sequence. A full length cDNA molecule can be generated by ligating suitable fragments, using well known techniques.

[0240] Alternatively, amplification techniques, such as those described above, can be useful for obtaining a full length coding sequence from a partial cDNA sequence. One such amplification technique is inverse PCR (see Triglia et al., Nucl. Acids Res. 16:8186, 1988), which uses restriction enzymes to generate a fragment in the known region of the gene. The fragment is then circularized by intramolecular ligation and used as a template for PCR with divergent primers derived from the known region. Within an alternative approach, sequences adjacent to a partial sequence may be retrieved by amplification with a primer to a linker sequence and a primer specific to a known region. The amplified sequences are typically subjected to a second round of amplification with the same linker primer and a second primer specific to the known region. A variation on this procedure, which employs two primers that initiate extension in opposite directions from the known sequence, is described in WO 96/38591. Another such technique is known as “rapid amplification of cDNA ends” or RACE. This technique involves the use of an internal primer and an external primer, which hybridizes to a polyA region or vector sequence, to identify sequences that are 5′ and 3′ of a known sequence. Additional techniques include capture PCR (Lagerstrom et al., PCR Methods Applic. 1:111-19, 1991) and walking PCR (Parker et al., Nucl. Acids. Res. 19:3055-60, 1991). Other methods employing amplification may also be employed to obtain a full length cDNA sequence.

[0241] In certain instances, it is possible to obtain a full length cDNA sequence by analysis of sequences provided in an expressed sequence tag (EST) database, such as that available from GenBank. Searches for overlapping ESTs may generally be performed using well known programs (e.g., NCBI BLAST searches), and such ESTs may be used to generate a contiguous full length sequence. Full length DNA sequences may also be obtained by analysis of genomic fragments.

[0242] In other embodiments of the invention, polynucleotide sequences or fragments thereof which encode polypeptides of the invention, or fusion proteins or functional equivalents thereof, may be used in recombinant DNA molecules to direct expression of a polypeptide in appropriate host cells. Due to the inherent degeneracy of the genetic code, other DNA sequences that encode substantially the same or a functionally equivalent amino acid sequence may be produced and these sequences may be used to clone and express a given polypeptide.

[0243] As will be understood by those of skill in the art, it may be advantageous in some instances to produce polypeptide-encoding nucleotide sequences possessing non-naturally occurring codons. For example, codons preferred by a particular prokaryotic or eukaryotic host can be selected to increase the rate of protein expression or to produce a recombinant RNA transcript having desirable properties, such as a half-life which is longer than that of a transcript generated from the naturally occurring sequence.

[0244] Moreover, the polynucleotide sequences of the present invention can be engineered using methods generally known in the art in order to alter polypeptide encoding sequences for a variety of reasons, including but not limited to, alterations which modify the cloning, processing, and/or expression of the gene product. For example, DNA shuffling by random fragmentation and PCR reassembly of gene fragments and synthetic oligonucleotides may be used to engineer the nucleotide sequences. In addition, site-directed mutagenesis may be used to insert new restriction sites, alter glycosylation patterns, change codon preference, produce splice variants, or introduce mutations, and so forth.

[0245] In another embodiment of the invention, natural, modified, or recombinant nucleic acid sequences may be ligated to a heterologous sequence to encode a fusion protein. For example, to screen peptide libraries for inhibitors of polypeptide activity, it may be useful to encode a chimeric protein that can be recognized by a commercially available antibody. A fusion protein may also be engineered to contain a cleavage site located between the polypeptide-encoding sequence and the heterologous protein sequence, so that the polypeptide may be cleaved and purified away from the heterologous moiety.

[0246] Sequences encoding a desired polypeptide may be synthesized, in whole or in part, using chemical methods well known in the art (see Caruthers, M. H. et al. (1980) Nucl. Acids Res. Symp. Ser. 215-223, Horn, T. et al. (1980) Nucl. Acids Res. Symp. Ser. 225-232). Alternatively, the protein itself may be produced using chemical methods to synthesize the amino acid sequence of a polypeptide, or a portion thereof. For example, peptide synthesis can be performed using various solid-phase techniques (Roberge, J. Y. et al. (1995) Science 269:202-204) and automated synthesis may be achieved, for example, using the ABI 431A Peptide Synthesizer (Perkin Elmer, Palo Alto, Calif.).

[0247] A newly synthesized peptide may be substantially purified by preparative high performance liquid chromatography (e.g., Creighton, T. (1983) Proteins, Structures and Molecular Principles, W H Freeman and Co., New York, N.Y.) or other comparable techniques available in the art. The composition of the synthetic peptides may be confirmed by amino acid analysis or sequencing (e.g., the Edman degradation procedure). Additionally, the amino acid sequence of a polypeptide, or any part thereof, may be altered during direct synthesis and/or combined using chemical methods with sequences from other proteins, or any part thereof, to produce a variant polypeptide.

[0248] In order to express a desired polypeptide, the nucleotide sequences encoding the polypeptide, or functional equivalents, may be inserted into appropriate expression vector, i.e., a vector which contains the necessary elements for the transcription and translation of the inserted coding sequence. Methods which are well known to those skilled in the art may be used to construct expression vectors containing sequences encoding a polypeptide of interest and appropriate transcriptional and translational control elements. These methods include in vitro recombinant DNA techniques, synthetic techniques, and in vivo genetic recombination. Such techniques are described, for example, in Sambrook, J. et al. (1989) Molecular Cloning, A Laboratory Manual, Cold Spring Harbor Press, Plainview, N.Y., and Ausubel, F. M. et al. (1989) Current Protocols in Molecular Biology, John Wiley & Sons, New York. N.Y.

[0249] A variety of expression vector/host systems may be utilized to contain and express polynucleotide sequences. These include, but are not limited to, microorganisms such as bacteria transformed with recombinant bacteriophage, plasmid, or cosmid DNA expression vectors; yeast transformed with yeast expression vectors; insect cell systems infected with virus expression vectors (e.g., baculovirus); plant cell systems transformed with virus expression vectors (e.g., cauliflower mosaic virus, CaMV; tobacco mosaic virus, TMV) or with bacterial expression vectors (e.g., Ti or pBR322 plasmids); or animal cell systems.

[0250] The “control elements” or “regulatory sequences” present in an expression vector are those non-translated regions of the vector-enhancers, promoters, 5′ and 3′ untranslated regions—which interact with host cellular proteins to carry out transcription and translation. Such elements may vary in their strength and specificity. Depending on the vector system and host utilized, any number of suitable transcription and translation elements, including constitutive and inducible promoters, may be used. For example, when cloning in bacterial systems, inducible promoters such as the hybrid lacZ promoter of the PBLUESCRIPT phagemid (Stratagene, La Jolla, Calif.) or PSPORT1 plasmid (Gibco BRL, Gaithersburg, Md.) and the like may be used. In mammalian cell systems, promoters from mammalian genes or from mammalian viruses are generally preferred. If it is necessary to generate a cell line that contains multiple copies of the sequence encoding a polypeptide, vectors based on SV40 or EBV may be advantageously used with an appropriate selectable marker.

[0251] In bacterial systems, any of a number of expression vectors may be selected depending upon the use intended for the expressed polypeptide. For example, when large quantities are needed, for example for the induction of antibodies, vectors which direct high level expression of fusion proteins that are readily purified may be used. Such vectors include, but are not limited to, the multifunctional E. coli cloning and expression vectors such as BLUESCRIPT (Stratagene), in which the sequence encoding the polypeptide of interest may be ligated into the vector in frame with sequences for the amino-terminal Met and the subsequent 7 residues of .beta.-galactosidase so that a hybrid protein is produced; pIN vectors (Van Heeke, G. and S. M. Schuster (1989) J. Biol. Chem. 264:5503-5509); and the like. pGEX Vectors (Promega, Madison, Wis.) may also be used to express foreign polypeptides as fusion proteins with glutathione S-transferase (GST). In general, such fusion proteins are soluble and can easily be purified from lysed cells by adsorption to glutathione-agarose beads followed by elution in the presence of free glutathione. Proteins made in such systems may be designed to include heparin, thrombin, or factor XA protease cleavage sites so that the cloned polypeptide of interest can be released from the GST moiety at will.

[0252] In the yeast, Saccharomyces cerevisiae, a number of vectors containing constitutive or inducible promoters such as alpha factor, alcohol oxidase, and PGH may be used. For reviews, see Ausubel et al. (supra) and Grant et al. (1987) Methods Enzymol. 153:516-544.

[0253] In cases where plant expression vectors are used, the expression of sequences encoding polypeptides may be driven by any of a number of promoters. For example, viral promoters such as the 35S and 19S promoters of CaMV may be used alone or in combination with the omega leader sequence from TMV (Takamatsu, N. (1987) EMBO J. 6:307-311. Alternatively, plant promoters such as the small subunit of RUBISCO or heat shock promoters may be used (Coruzzi, G. et al. (1984) EMBO J. 3:1671-1680; Broglie, R. et al. (1984) Science 224:838-843; and Winter, J. et al. (1991) Results Probl. Cell Differ. 17:85-105). These constructs can be introduced into plant cells by direct DNA transformation or pathogen-mediated transfection. Such techniques are described in a number of generally available reviews (see, for example, Hobbs, S. or Murry, L. E. in McGraw Hill Yearbook of Science and Technology (1992) McGraw Hill, New York, N.Y.; pp. 191-196).

[0254] An insect system may also be used to express a polypeptide of interest. For example, in one such system, Autographa californica nuclear polyhedrosis virus (AcNPV) is used as a vector to express foreign genes in Spodoptera frugiperda cells or in Trichoplusia larvae. The sequences encoding the polypeptide may be cloned into a non-essential region of the virus, such as the polyhedrin gene, and placed under control of the polyhedrin promoter. Successful insertion of the polypeptide-encoding sequence will render the polyhedrin gene inactive and produce recombinant virus lacking coat protein. The recombinant viruses may then be used to infect, for example, S. frugiperda cells or Trichoplusia larvae in which the polypeptide of interest may be expressed (Engelhard, E. K. et al. (1994) Proc. Natl. Acad. Sci. 91 :3224-3227).

[0255] In mammalian host cells, a number of viral-based expression systems are generally available. For example, in cases where an adenovirus is used as an expression vector, sequences encoding a polypeptide of interest may be ligated into an adenovirus transcription/translation complex consisting of the late promoter and tripartite leader sequence. Insertion in a non-essential E1 or E3 region of the viral genome may be used to obtain a viable virus which is capable of expressing the polypeptide in infected host cells (Logan, J. and Shenk, T. (1984) Proc. Natl. Acad. Sci. 81:3655-3659). In addition, transcription enhancers, such as the Rous sarcoma virus (RSV) enhancer, may be used to increase expression in mammalian host cells.

[0256] Specific initiation signals may also be used to achieve more efficient translation of sequences encoding a polypeptide of interest. Such signals include the ATG initiation codon and adjacent sequences. In cases where sequences encoding the polypeptide, its initiation codon, and upstream sequences are inserted into the appropriate expression vector, no additional transcriptional or translational control signals may be needed. However, in cases where only coding sequence, or a portion thereof, is inserted, exogenous translational control signals including the ATG initiation codon should be provided. Furthermore, the initiation codon should be in the correct reading frame to ensure translation of the entire insert. Exogenous translational elements and initiation codons may be of various origins, both natural and synthetic. The efficiency of expression may be enhanced by the inclusion of enhancers which are appropriate for the particular cell system which is used, such as those described in the literature (Scharf, D. et al. (1994) Results Probl. Cell Differ. 20:125-162).

[0257] In addition, a host cell strain may be chosen for its ability to modulate the expression of the inserted sequences or to process the expressed protein in the desired fashion. Such modifications of the polypeptide include, but are not limited to, acetylation, carboxylation. glycosylation, phosphorylation, lipidation, and acylation. Post-translational processing which cleaves a “prepro” form of the protein may also be used to facilitate correct insertion, folding and/or function. Different host cells such as CHO, COS, HeLa, MDCK, HEK293, and W138, which have specific cellular machinery and characteristic mechanisms for such post-translational activities, may be chosen to ensure the correct modification and processing of the foreign protein.

[0258] For long-term, high-yield production of recombinant proteins, stable expression is generally preferred. For example, cell lines which stably express a polynucleotide of interest may be transformed using expression vectors which may contain viral origins of replication and/or endogenous expression elements and a selectable marker gene on the same or on a separate vector. Following the introduction of the vector, cells may be allowed to grow for 1-2 days in an enriched media before they are switched to selective media. The purpose of the selectable marker is to confer resistance to selection, and its presence allows growth and recovery of cells which successfully express the introduced sequences. Resistant clones of stably transformed cells may be proliferated using tissue culture techniques appropriate to the cell type.

[0259] Any number of selection systems may be used to recover transformed cell lines. These include, but are not limited to, the herpes simplex virus thymidine kinase (Wigler, M. et al. (1977) Cell 11:223-32) and adenine phosphoribosyltransferase (Lowy, I. et al. (1990) Cell 22:817-23) genes which can be employed in tk.sup.- or aprt.sup.- cells, respectively. Also, antimetabolite, antibiotic or herbicide resistance can be used as the basis for selection; for example, dhfr which confers resistance to methotrexate (Wigler, M. et al. (1980) Proc. Natl. Acad. Sci. 77:3567-70); npt, which confers resistance to the aminoglycosides, neomycin and G-418 (Colbere-Garapin, F. et al (1981) J. Mol. Biol. 150:1-14); and als or pat, which confer resistance to chlorsulfuron and phosphinotricin acetyltransferase, respectively (Murry, supra). Additional selectable genes have been described, for example, trpB, which allows cells to utilize indole in place of tryptophan, or hisD, which allows cells to utilize histinol in place of histidine (Hartman, S. C. and R. C. Mulligan (1988) Proc. Natl. Acad. Sci. 85:8047-51). The use of visible markers has gained popularity with such markers as anthocyanins, beta-glucuronidase and its substrate GUS, and luciferase and its substrate luciferin, being widely used not only to identify transformants, but also to quantify the amount of transient or stable protein expression attributable to a specific vector system (Rhodes, C. A. et al. (1995) Methods Mol. Biol. 55:121-131).

[0260] Although the presence/absence of marker gene expression suggests that the gene of interest is also present, its presence and expression may need to be confirmed. For example, if the sequence encoding a polypeptide is inserted within a marker gene sequence, recombinant cells containing sequences can be identified by the absence of marker gene function. Alternatively, a marker gene can be placed in tandem with a polypeptide-encoding sequence under the control of a single promoter. Expression of the marker gene in response to induction or selection usually indicates expression of the tandem gene as well.

[0261] Alternatively, host cells that contain and express a desired polynucleotide sequence may be identified by a variety of procedures known to those of skill in the art. These procedures include, but are not limited to, DNA-DNA or DNA-RNA hybridizations and protein bioassay or immunoassay techniques which include, for example, membrane, solution, or chip based technologies for the detection and/or quantification of nucleic acid or protein.

[0262] A variety of protocols for detecting and measuring the expression of polynucleotide-encoded products, using either polyclonal or monoclonal antibodies specific for the product are known in the art. Examples include enzyme-linked immunosorbent assay (ELISA), radioimmunoassay (RIA), and fluorescence activated cell sorting (FACS). A two-site, monoclonal-based immunoassay utilizing monoclonal antibodies reactive to two non-interfering epitopes on a given polypeptide may be preferred for some applications, but a competitive binding assay may also be employed. These and other assays are described, among other places, in Hampton, R. et al. (1990; Serological Methods, a Laboratory Manual, APS Press, St. Paul, Minn.) and Maddox, D. E. et al. (1983; J. Exp. Med. 158:1211-1216).

[0263] A wide variety of labels and conjugation techniques are known by those skilled in the art and may be used in various nucleic acid and amino acid assays. Means for producing labeled hybridization or PCR probes for detecting sequences related to polynucleotides include oligolabeling, nick translation, end-labeling or PCR amplification using a labeled nucleotide. Alternatively, the sequences, or any portions thereof may be cloned into a vector for the production of an mRNA probe. Such vectors are known in the art, are commercially available, and may be used to synthesize RNA probes in vitro by addition of an appropriate RNA polymerase such as T7, T3, or SP6 and labeled nucleotides. These procedures may be conducted using a variety of commercially available kits. Suitable reporter molecules or labels, which may be used include radionuclides, enzymes, fluorescent, chemiluminescent, or chromogenic agents as well as substrates, cofactors, inhibitors, magnetic particles, and the like.

[0264] Host cells transformed with a polynucleotide sequence of interest may be cultured under conditions suitable for the expression and recovery of the protein from cell culture. The protein produced by a recombinant cell may be secreted or contained intracellularly depending on the sequence and/or the vector used. As will be understood by those of skill in the art, expression vectors containing polynucleotides of the invention may be designed to contain signal sequences which direct secretion of the encoded polypeptide through a prokaryotic or eukaryotic cell membrane. Other recombinant constructions may be used to join sequences encoding a polypeptide of interest to nucleotide sequence encoding a polypeptide domain which will facilitate purification of soluble proteins. Such purification facilitating domains include, but are not limited to, metal chelating peptides such as histidine-tryptophan modules that allow purification on immobilized metals, protein A domains that allow purification on immobilized immunoglobulin, and the domain utilized in the FLAGS extension/affinity purification system (Immunex Corp., Seattle, Wash.). The inclusion of cleavable linker sequences such as those specific for Factor XA or enterokinase (Invitrogen. San Diego, Calif.) between the purification domain and the encoded polypeptide may be used to facilitate purification. One such expression vector provides for expression of a fusion protein containing a polypeptide of interest and a nucleic acid encoding 6 histidine residues preceding a thioredoxin or an enterokinase cleavage site. The histidine residues facilitate purification on IMIAC (immobilized metal ion affinity chromatography) as described in Porath, J. et al. (1992, Prot. Exp. Purif 3:263-281) while the enterokinase cleavage site provides a means for purifying the desired polypeptide from the fusion protein. A discussion of vectors which contain fusion proteins is provided in Kroll, D. J. et al. (1993; DNA Cell Biol. 12:441-453).

[0265] In addition to recombinant production methods, polypeptides of the invention, and fragments thereof, may be produced by direct peptide synthesis using solid-phase techniques (Merrifield J. (1963) J. Am. Chem. Soc. 85:2149-2154). Protein synthesis may be performed using manual techniques or by automation. Automated synthesis may be achieved, for example, using Applied Biosystems 431A Peptide Synthesizer (Perkin Elmer). Alternatively, various fragments may be chemically synthesized separately and combined using chemical methods to produce the full length molecule.

[0266] Antibody Compositions, Fragments Thereof and Other Binding Agents

[0267] According to another aspect, the present invention further provides binding agents, such as antibodies and antigen-binding fragments thereof, that exhibit immunological binding to a tumor polypeptide disclosed herein, or to a portion, variant or derivative thereof. An antibody, or antigen-binding fragment thereof, is said to “specifically bind,” “immunogically bind,” and/or is “immunologically reactive” to a polypeptide of the invention if it reacts at a detectable level (within, for example, an ELISA assay) with the polypeptide, and does not react detectably with unrelated polypeptides under similar conditions.

[0268] Immunological binding, as used in this context, generally refers to the non-covalent interactions of the type which occur between an immunoglobulin molecule and an antigen for which the immunoglobulin is specific. The strength, or affinity of immunological binding interactions can be expressed in terms of the dissociation constant (K_(d)) of the interaction, wherein a smaller K_(d) represents a greater affinity. Immunological binding properties of selected polypeptides can be quantified using methods well known in the art. One such method entails measuring the rates of antigen-binding site/antigen complex formation and dissociation, wherein those rates depend on the concentrations of the complex partners, the affinity of the interaction, and on geometric parameters that equally influence the rate in both directions. Thus, both the “on rate constant” (K_(on)) and the “off rate constant” (K_(off)) can be determined by calculation of the concentrations and the actual rates of association and dissociation. The ratio of K_(off)/K_(on) enables cancellation of all parameters not related to affinity, and is thus equal to the dissociation constant K_(d). See, generally, Davies et al. (1990) Annual Rev. Biochem. 59:439-473.

[0269] An “antigen-binding site,” or “binding portion” of an antibody refers to the part of the immunoglobulin molecule that participates in antigen binding. The antigen binding site is formed by amino acid residues of the N-terminal variable (“V”) regions of the heavy (“H”) and light (“L”) chains. Three highly divergent stretches within the V regions of the heavy and light chains are referred to as “hypervariable regions” which are interposed between more conserved flanking stretches known as “framework regions,” or “FRs”. Thus the term “FR” refers to amino acid sequences which are naturally found between and adjacent to hypervariable regions in immunoglobulins. In an antibody molecule, the three hypervariable regions of a light chain and the three hypervariable regions of a heavy chain are disposed relative to each other in three dimensional space to form an antigen-binding surface. The antigen-binding surface is complementary to the three-dimensional surface of a bound antigen, and the three hypervariable regions of each of the heavy and light chains are referred to as “complementarity-determining regions,” or “CDRs.”

[0270] Binding agents may be further capable of differentiating between patients with and without a cancer, such as ovarian cancer, using the representative assays provided herein. For example, antibodies or other binding agents that bind to a tumor protein will preferably generate a signal indicating the presence of a cancer in at least about 20% of patients with the disease, more preferably at least about 30% of patients. Alternatively, or in addition, the antibody will generate a negative signal indicating the absence of the disease in at least about 90% of individuals without the cancer. To determine whether a binding agent satisfies this requirement, biological samples (e.g., blood, sera, sputum, urine and/or tumor biopsies) from patients with and without a cancer (as determined using standard clinical tests) may be assayed as described herein for the presence of polypeptides that bind to the binding agent. Preferably, a statistically significant number of samples with and without the disease will be assayed. Each binding agent should satisfy the above criteria; however, those of ordinary skill in the art will recognize that binding agents may be used in combination to improve sensitivity.

[0271] Any agent that satisfies the above requirements may be a binding agent. For example, a binding agent may be a ribosome, with or without a peptide component, an RNA molecule or a polypeptide. In a preferred embodiment, a binding agent is an antibody or an antigen-binding fragment thereof. Antibodies may be prepared by any of a variety of techniques known to those of ordinary skill in the art. See, e.g., Harlow and Lane, Antibodies: A Laboratory Manual, Cold Spring Harbor Laboratory, 1988. In general, antibodies can be produced by cell culture techniques, including the generation of monoclonal antibodies as described herein, or via transfection of antibody genes into suitable bacterial or mammalian cell hosts, in order to allow for the production of recombinant antibodies. In one technique, an immunogen comprising the polypeptide is initially injected into any of a wide variety of mammals (e.g., mice, rats, rabbits, sheep or goats). In this step, the polypeptides of this invention may serve as the immunogen without modification. Alternatively, particularly for relatively short polypeptides, a superior immune response may be elicited if the polypeptide is joined to a carrier protein, such as bovine serum albumin or keyhole limpet hemocyanin. The immunogen is injected into the animal host, preferably according to a predetermined schedule incorporating one or more booster immunizations, and the animals are bled periodically. Polyclonal antibodies specific for the polypeptide may then be purified from such antisera by, for example, affinity chromatography using the polypeptide coupled to a suitable solid support.

[0272] Monoclonal antibodies specific for an antigenic polypeptide of interest may be prepared, for example, using the technique of Kohler and Milstein, Eur. J. Immunol. 6:511-519, 1976, and improvements thereto. Briefly, these methods involve the preparation of immortal cell lines capable of producing antibodies having the desired specificity (i.e., reactivity with the polypeptide of interest). Such cell lines may be produced, for example, from spleen cells obtained from an animal immunized as described above. The spleen cells are then immortalized by, for example, fusion with a myeloma cell fusion partner, preferably one that is syngeneic with the immunized animal. A variety of fusion techniques may be employed. For example, the spleen cells and myeloma cells may be combined with a nonionic detergent for a few minutes and then plated at low density on a selective medium that supports the growth of hybrid cells, but not myeloma cells. A preferred selection technique uses HAT (hypoxanthine, aminopterin, thymidine) selection. After a sufficient time, usually about 1 to 2 weeks, colonies of hybrids are observed. Single colonies are selected and their culture supernatants tested for binding activity against the polypeptide. Hybridomas having high reactivity and specificity are preferred.

[0273] Monoclonal antibodies may be isolated from the supernatants of growing hybridoma colonies. In addition, various techniques may be employed to enhance the yield, such as injection of the hybridoma cell line into the peritoneal cavity of a suitable vertebrate host, such as a mouse. Monoclonal antibodies may then be harvested from the ascites fluid or the blood. Contaminants may be removed from the antibodies by conventional techniques, such as chromatography, gel filtration, precipitation, and extraction. The polypeptides of this invention may be used in the purification process in, for example, an affinity chromatography step.

[0274] A number of therapeutically useful molecules are known in the art which comprise antigen-binding sites that are capable of exhibiting immunological binding properties of an antibody molecule. The proteolytic enzyme papain preferentially cleaves IgG molecules to yield several fragments, two of which (the “F(ab)” fragments) each comprise a covalent heterodimer that includes an intact antigen-binding site. The enzyme pepsin is able to cleave IgG molecules to provide several fragments, including the “F(ab′)₂” fragment which comprises both antigen-binding sites. An “Fv” fragment can be produced by preferential proteolytic cleavage of an IgM, and on rare occasions IgG or IgA immunoglobulin molecule. Fv fragments are, however, more commonly derived using recombinant techniques known in the art. The Fv fragment includes a non-covalent V_(H)::V_(L) heterodimer including an antigen-binding site which retains much of the antigen recognition and binding capabilities of the native antibody molecule. Inbar et al. (1972) Proc. Nat. Acad. Sci. USA 69:2659-2662; Hochman et al. (1976) Biochem 15:2706-2710; and Ehrlich et al. (1980) Biochem 19:4091-4096.

[0275] A single chain Fv (“sFv”) polypeptide is a covalently linked V_(H)::V_(L) heterodimer which is expressed from a gene fusion including V_(H)- and V_(L)-encoding genes linked by a peptide-encoding linker. Huston et al. (1988) Proc. Nat. Acad. Sci. USA 85(16):5879-5883. A number of methods have been described to discern chemical structures for converting the naturally aggregated—but chemically separated—light and heavy polypeptide chains from an antibody V region into an sFv molecule which will fold into a three dimensional structure substantially similar to the structure of an antigen-binding site. See, e.g., U.S. Pat. Nos. 5,091,513 and 5,132,405, to Huston et al.; and U.S. Pat. No. 4,946,778, to Ladner et al.

[0276] Each of the above-described molecules includes a heavy chain and a light chain CDR set, respectively interposed between a heavy chain and a light chain FR set which provide support to the CDRS and define the spatial relationship of the CDRs relative to each other. As used herein, the term “CDR set” refers to the three hypervariable regions of a heavy or light chain V region. Proceeding from the N-terminus of a heavy or light chain, these regions are denoted as “CDR1,” “CDR2,” and “CDR3” respectively. An antigen-binding site, therefore, includes six CDRs, comprising the CDR set from each of a heavy and a light chain V region. A polypeptide comprising a single CDR, (e.g., a CDR1, CDR2 or CDR3) is referred to herein as a “molecular recognition unit.” Crystallographic analysis of a number of antigen-antibody complexes has demonstrated that the amino acid residues of CDRs form extensive contact with bound antigen, wherein the most extensive antigen contact is with the heavy chain CDR3. Thus, the molecular recognition units are primarily responsible for the specificity of an antigen-binding site.

[0277] As used herein, the term “FR set” refers to the four flanking amino acid sequences which frame the CDRs of a CDR set of a heavy or light chain V region. Some FR residues may contact bound antigen; however, FRs are primarily responsible for folding the V region into the antigen-binding site, particularly the FR residues directly adjacent to the CDRS. Within FRs, certain amino residues and certain structural features are very highly conserved. In this regard, all V region sequences contain an internal disulfide loop of around 90 amino acid residues. When the V regions fold into a binding-site, the CDRs are displayed as projecting loop motifs which form an antigen-binding surface. It is generally recognized that there are conserved structural regions of FRs which influence the folded shape of the CDR loops into certain “canonical” structures—regardless of the precise CDR amino acid sequence. Further, certain FR residues are known to participate in non-covalent interdomain contacts which stabilize the interaction of the antibody heavy and light chains.

[0278] A number of “humanized” antibody molecules comprising an antigen-binding site derived from a non-human immunoglobulin have been described, including chimeric antibodies having rodent V regions and their associated CDRs fused to human constant domains (Winter et al. (1991) Nature 349:293-299; Lobuglio et al. (1989) Proc. Nat. Acad. Sci. USA 86:4220-4224; Shaw et al. (1987) J Immunol. 138:4534-4538; and Brown et al. (1987) Cancer Res. 47:3577-3583), rodent CDRs grafted into a human supporting FR prior to fusion with an appropriate human antibody constant domain (Riechmann et al. (1988) Nature 332:323-327; Verhoeyen et al. (1988) Science 239:1534-1536; and Jones et al. (1986) Nature 321:522-525), and rodent CDRs supported by recombinantly veneered rodent FRs (European Patent Publication No. 519,596, published Dec. 23, 1992). These “humanized” molecules are designed to minimize unwanted immunological response toward rodent antihuman antibody molecules which limits the duration and effectiveness of therapeutic applications of those moieties in human recipients.

[0279] As used herein, the terms “veneered FRs” and “recombinantly veneered FRs” refer to the selective replacement of FR residues from, e.g., a rodent heavy or light chain V region, with human FR residues in order to provide a xenogeneic molecule comprising an antigen-binding site which retains substantially all of the native FR polypeptide folding structure. Veneering techniques are based on the understanding that the ligand binding characteristics of an antigen-binding site are determined primarily by the structure and relative disposition of the heavy and light chain CDR sets within the antigen-binding surface. Davies et al. (1990) Ann. Rev. Biochem. 59:439-473. Thus, antigen binding specificity can be preserved in a humanized antibody only wherein the CDR structures, their interaction with each other, and their interaction with the rest of the V region domains are carefully maintained. By using veneering techniques, exterior (e.g., solvent-accessible) FR residues which are readily encountered by the immune system are selectively replaced with human residues to provide a hybrid molecule that comprises either a weakly immunogenic, or substantially non-immunogenic veneered surface.

[0280] The process of veneering makes use of the available sequence data for human antibody variable domains compiled by Kabat et al., in Sequences of Proteins of Immunological Interest, 4th ed., (U.S. Dept. of Health and Human Services, U.S. Government Printing Office, 1987), updates to the Kabat database, and other accessible U.S. and foreign databases (both nucleic acid and protein). Solvent accessibilities of V region amino acids can be deduced from the known three-dimensional structure for human and murine antibody fragments. There are two general steps in veneering a murine antigen-binding site. Initially, the FRs of the variable domains of an antibody molecule of interest are compared with corresponding FR sequences of human variable domains obtained from the above-identified sources. The most homologous human V regions are then compared residue by residue to corresponding murine amino acids. The residues in the murine FR which differ from the human counterpart are replaced by the residues present in the human moiety using recombinant techniques well known in the art. Residue switching is only carried out with moieties which are at least partially exposed (solvent accessible), and care is exercised in the replacement of amino acid residues which may have a significant effect on the tertiary structure of V region domains, such as proline, glycine and charged amino acids.

[0281] In this manner, the resultant “veneered” murine antigen-binding sites are thus designed to retain the murine CDR residues, the residues substantially adjacent to the CDRs, the residues identified as buried or mostly buried (solvent inaccessible), the residues believed to participate in non-covalent (e.g., electrostatic and hydrophobic) contacts between heavy and light chain domains, and the residues from conserved structural regions of the FRs which are believed to influence the “canonical” tertiary structures of the CDR loops. These design criteria are then used to prepare recombinant nucleotide sequences which combine the CDRs of both the heavy and light chain of a murine antigen-binding site into human-appearing FRs that can be used to transfect mammalian cells for the expression of recombinant human antibodies which exhibit the antigen specificity of the murine antibody molecule.

[0282] In another embodiment of the invention, monoclonal antibodies of the present invention may be coupled to one or more therapeutic agents. Suitable agents in this regard include radionuclides, differentiation inducers, drugs, toxins, and derivatives thereof. Preferred radionuclides include ⁹⁰Y, ¹²³I, ¹²⁵I, ¹³¹I, ¹⁸⁶Re, ¹⁸⁸Re, ²¹¹At, and ²¹²Bi. Preferred drugs include methotrexate, and pyrimidine and purine analogs. Preferred differentiation inducers include phorbol esters and butyric acid. Preferred toxins include ricin, abrin, diptheria toxin, cholera toxin, gelonin Pseudomonas exotoxin, Shigella toxin, and pokeweed antiviral protein.

[0283] A therapeutic agent may be coupled (e.g., covalently bonded) to a suitable monoclonal antibody either directly or indirectly (e.g., via a linker group). A direct reaction between an agent and an antibody is possible when each possesses a substituent capable of reacting with the other. For example, a nucleophilic group, such as an amino or sulfhydryl group, on one may be capable of reacting with a carbonyl-containing group, such as an anhydride or an acid halide, or with an alkyl group containing a good leaving group (e.g., a halide) on the other.

[0284] Alternatively, it may be desirable to couple a therapeutic agent and an antibody via a linker group. A linker group can function as a spacer to distance an antibody from an agent in order to avoid interference with binding capabilities. A linker group can also serve to increase the chemical reactivity of a substituent on an agent or an antibody, and thus increase the coupling efficiency. An increase in chemical reactivity may also facilitate the use of agents, or functional groups on agents, which otherwise would not be possible.

[0285] It will be evident to those skilled in the art that a variety of bifunctional or polyfunctional reagents, both homo- and hetero-functional (such as those described in the catalog of the Pierce Chemical Co., Rockford, Ill.), may be employed as the linker group. Coupling may be effected, for example, through amino groups, carboxyl groups, sulfhydryl groups or oxidized carbohydrate residues. There are numerous references describing such methodology, e.g., U.S. Pat. No. 4,671,958, to Rodwell et al.

[0286] Where a therapeutic agent is more potent when free from the antibody portion of the immunoconjugates of the present invention, it may be desirable to use a linker group which is cleavable during or upon internalization into a cell. A number of different cleavable linker groups have been described. The mechanisms for the intracellular release of an agent from these linker groups include cleavage by reduction of a disulfide bond (e.g., U.S. Pat. No. 4,489,710, to Spitler) by irradiation of a photolabile bond (e.g., U.S. Pat. No. 4,625,014, to Senter et al.), by hydrolysis of derivatized amino acid side chains (e.g., U.S. Pat. No. 4,638,045, to Kohn et al.), by serum complement-mediated hydrolysis (e.g., U.S. Pat. No. 4,671,958, to Rodwell et al.), and acid-catalyzed hydrolysis (e.g., U.S. Pat. No. 4,569,789, to Blattler et al.).

[0287] It may be desirable to couple more than one agent to an antibody. In one embodiment, multiple molecules of an agent are coupled to one antibody molecule. In another embodiment, more than one type of agent may be coupled to one antibody. Regardless of the particular embodiment, immunoconjugates with more than one agent may be prepared in a variety of ways. For example, more than one agent may be coupled directly to an antibody molecule, or linkers that provide multiple sites for attachment can be used. Alternatively, a carrier can be used.

[0288] A carrier may bear the agents in a variety of ways, including covalent bonding either directly or via a linker group. Suitable carriers include proteins such as albumins (e.g., U.S. Pat. No. 4,507,234, to Kato et al.), peptides and polysaccharides such as aminodextran (e.g., U.S. Pat. No. 4,699,784, to Shih et al.). A carrier may also bear an agent by noncovalent bonding or by encapsulation, such as within a liposome vesicle (e.g., U.S. Pat. Nos. 4,429,008 and 4,873,088). Carriers specific for radionuclide agents include radiohalogenated small molecules and chelating compounds. For example, U.S. Pat. No. 4,735,792 discloses representative radiohalogenated small molecules and their synthesis. A radionuclide chelate may be formed from chelating compounds that include those containing nitrogen and sulfur atoms as the donor atoms for binding the metal, or metal oxide, radionuclide. For example, U.S. Pat. No. 4,673,562, to Davison et al. discloses representative chelating compounds and their synthesis.

[0289] T Cell Compositions

[0290] The present invention, in another aspect, provides T cells specific for a tumor polypeptide disclosed herein, or for a variant or derivative thereof. Such cells may generally be prepared in vitro or ex vivo, using standard procedures. For example, T cells may be isolated from bone marrow, peripheral blood, or a fraction of bone marrow or peripheral blood of a patient, using a commercially available cell separation system, such as the Isolex™ System, available from Nexell Therapeutics, Inc. (Irvine, Calif.; see also U.S. Pat. No. 5,240,856; U.S. Pat. No. 5,215,926; WO 89/06280; WO 91/16116 and WO 92/07243). Alternatively, T cells may be derived from related or unrelated humans, non-human mammals, cell lines or cultures.

[0291] T cells may be stimulated with a polypeptide, polynucleotide encoding a polypeptide and/or an antigen presenting cell (APC) that expresses such a polypeptide. Such stimulation is performed under conditions and for a time sufficient to permit the generation of T cells that are specific for the polypeptide of interest. Preferably, a tumor polypeptide or polynucleotide of the invention is present within a delivery vehicle, such as a microsphere, to facilitate the generation of specific T cells.

[0292] T cells are considered to be specific for a polypeptide of the present invention if the T cells specifically proliferate, secrete cytokines or kill target cells coated with the polypeptide or expressing a gene encoding the polypeptide. T cell specificity may be evaluated using any of a variety of standard techniques. For example, within a chromium release assay or proliferation assay, a stimulation index of more than two fold increase in lysis and/or proliferation, compared to negative controls, indicates T cell specificity. Such assays may be performed, for example, as described in Chen et al., Cancer Res. 54:1065-1070, 1994. Alternatively, detection of the proliferation of T cells may be accomplished by a variety of known techniques. For example, T cell proliferation can be detected by measuring an increased rate of DNA synthesis (e.g., by pulse-labeling cultures of T cells with tritiated thymidine and measuring the amount of tritiated thymidine incorporated into DNA). Contact with a tumor polypeptide (100 ng/ml-100 μg/ml, preferably 200 ng/ml-25 μg/ml) for 3-7 days will typically result in at least a two fold increase in proliferation of the T cells. Contact as described above for 2-3 hours should result in activation of the T cells, as measured using standard cytokine assays in which a two fold increase in the level of cytokine release (e.g., TNF or IFN-γ) is indicative of T cell activation (see Coligan et al., Current Protocols in Immunology, vol. 1, Wiley Interscience (Greene 1998)). T cells that have been activated in response to a tumor polypeptide, polynucleotide or polypeptide-expressing APC may be CD4⁺ and/or CD8⁺. Tumor polypeptide-specific T cells may be expanded using standard techniques. Within preferred embodiments, the T cells are derived from a patient, a related donor or an unrelated donor, and are administered to the patient following stimulation and expansion.

[0293] For therapeutic purposes, CD4⁺ or CD8⁺ T cells that proliferate in response to a tumor polypeptide, polynucleotide or APC can be expanded in number either in vitro or in vivo. Proliferation of such T cells in vitro may be accomplished in a variety of ways. For example, the T cells can be re-exposed to a tumor polypeptide, or a short peptide corresponding to an immunogenic portion of such a polypeptide, with or without the addition of T cell growth factors, such as interleukin-2, and/or stimulator cells that synthesize a tumor polypeptide. Alternatively, one or more T cells that proliferate in the presence of the tumor polypeptide can be expanded in number by cloning. Methods for cloning cells are well known in the art, and include limiting dilution.

[0294] Pharmaceutical Compositions

[0295] In additional embodiments, the present invention concerns formulation of one or more of the polynucleotide, polypeptide, T-cell and/or antibody compositions disclosed herein in pharmaceutically-acceptable carriers for administration to a cell or an animal, either alone, or in combination with one or more other modalities of therapy.

[0296] It will be understood that, if desired, a composition as disclosed herein may be administered in combination with other agents as well, such as, e.g., other proteins or polypeptides or various pharmaceutically-active agents. In fact, there is virtually no limit to other components that may also be included, given that the additional agents do not cause a significant adverse effect upon contact with the target cells or host tissues. The compositions may thus be delivered along with various other agents as required in the particular instance. Such compositions may be purified from host cells or other biological sources, or alternatively may be chemically synthesized as described herein. Likewise, such compositions may further comprise substituted or derivatized RNA or DNA compositions.

[0297] Therefore, in another aspect of the present invention, pharmaceutical compositions are provided comprising one or more of the polynucleotide, polypeptide, antibody, and/or T-cell compositions described herein in combination with a physiologically acceptable carrier. In certain preferred embodiments, the pharmaceutical compositions of the invention comprise immunogenic polynucleotide and/or polypeptide compositions of the invention for use in prophylactic and therapeutic vaccine applications. Vaccine preparation is generally described in, for example, M. F. Powell and M. J. Newman, eds., “Vaccine Design (the subunit and adjuvant approach),” Plenum Press (NY, 1995). Generally, such compositions will comprise one or more polynucleotide and/or polypeptide compositions of the present invention in combination with one or more immunostimulants.

[0298] It will be apparent that any of the pharmaceutical compositions described herein can contain pharmaceutically acceptable salts of the polynucleotides and polypeptides of the invention. Such salts can be prepared, for example, from pharmaceutically acceptable non-toxic bases, including organic bases (e.g., salts of primary, secondary and tertiary amines and basic amino acids) and inorganic bases (e.g., sodium, potassium, lithium, ammonium, calcium and magnesium salts).

[0299] In another embodiment, illustrative immunogenic compositions, e.g., vaccine compositions, of the present invention comprise DNA encoding one or more of the polypeptides as described above, such that the polypeptide is generated in situ. As noted above, the polynucleotide may be administered within any of a variety of delivery systems known to those of ordinary skill in the art. Indeed, numerous gene delivery techniques are well known in the art, such as those described by Rolland, Crit. Rev. Therap. Drug Carrier Systems 15:143-198, 1998, and references cited therein. Appropriate polynucleotide expression systems will, of course, contain the necessary regulatory DNA regulatory sequences for expression in a patient (such as a suitable promoter and terminating signal). Alternatively, bacterial delivery systems may involve the administration of a bacterium (such as Bacillus-Calmette-Guerrin) that expresses an immunogenic portion of the polypeptide on its cell surface or secretes such an epitope.

[0300] Therefore, in certain embodiments, polynucleotides encoding immunogenic polypeptides described herein are introduced into suitable mammalian host cells for expression using any of a number of known viral-based systems. In one illustrative embodiment, retroviruses provide a convenient and effective platform for gene delivery systems. A selected nucleotide sequence encoding a polypeptide of the present invention can be inserted into a vector and packaged in retroviral particles using techniques known in the art. The recombinant virus can then be isolated and delivered to a subject. A number of illustrative retroviral systems have been described (e.g., U.S. Pat. No. 5,219,740; Miller and Rosman (1989) BioTechniques 7:980-990; Miller, A. D. (1990) Human Gene Therapy 1:5-14; Scarpa et al. (1991) Virology 180:849-852; Burns et al. (1993) Proc. Natl. Acad. Sci. USA 90:8033-8037; and Boris-Lawrie and Temin (1993) Cur. Opin. Genet. Develop. 3:102-109.

[0301] In addition, a number of illustrative adenovirus-based systems have also been described. Unlike retroviruses which integrate into the host genome, adenoviruses persist extrachromosomally thus minimizing the risks associated with insertional mutagenesis (Haj-Ahmad and Graham (1986) J. Virol. 57:267-274; Bett et al. (1993) J. Virol. 67:5911-5921; Mittereder et al. (1994) Human Gene Therapy 5:717-729; Seth et al. (1994) J. Virol. 68:933-940; Barr et al. (1994) Gene Therapy 1:51-58; Berkner, K. L. (1988) BioTechniques 6:616-629; and Rich et al. (1993) Human Gene Therapy 4:461-476).

[0302] Various adeno-associated virus (AAV) vector systems have also been developed for polynucleotide delivery. AAV vectors can be readily constructed using techniques well known in the art. See, e.g., U.S. Pat. Nos. 5,173,414 and 5,139,941; International Publication Nos. WO 92/01070 and WO 93/03769; Lebkowski et al. (1988) Molec. Cell. Biol. 8:3988-3996; Vincent et al. (1990) Vaccines 90 (Cold Spring Harbor Laboratory Press); Carter, B. J. (1992) Current Opinion in Biotechnology 3:533-539; Muzyczka, N. (1992) Current Topics in Microbiol. and Immunol. 158:97-129; Kotin, R. M. (1994) Human Gene Therapy 5:793-801; Shelling and Smith (1994) Gene Therapy 1:165-169; and Zhou et al. (1994) J. Exp. Med. 179:1867-1875.

[0303] Additional viral vectors useful for delivering the polynucleotides encoding polypeptides of the present invention by gene transfer include those derived from the pox family of viruses, such as vaccinia virus and avian poxvirus. By way of example, vaccinia virus recombinants expressing the novel molecules can be constructed as follows. The DNA encoding a polypeptide is first inserted into an appropriate vector so that it is adjacent to a vaccinia promoter and flanking vaccinia DNA sequences, such as the sequence encoding thymidine kinase (TK). This vector is then used to transfect cells which are simultaneously infected with vaccinia. Homologous recombination serves to insert the vaccinia promoter plus the gene encoding the polypeptide of interest into the viral genome. The resulting TK.sup.(-) recombinant can be selected by culturing the cells in the presence of 5-bromodeoxyuridine and picking viral plaques resistant thereto.

[0304] A vaccinia-based infection/transfection system can be conveniently used to provide for inducible, transient expression or coexpression of one or more polypeptides described herein in host cells of an organism. In this particular system, cells are first infected in vitro with a vaccinia virus recombinant that encodes the bacteriophage T7 RNA polymerase. This polymerase displays exquisite specificity in that it only transcribes templates bearing T7 promoters. Following infection, cells are transfected with the polynucleotide or polynucleotides of interest, driven by a T7 promoter. The polymerase expressed in the cytoplasm from the vaccinia virus recombinant transcribes the transfected DNA into RNA which is then translated into polypeptide by the host translational machinery. The method provides for high level, transient, cytoplasmic production of large quantities of RNA and its translation products. See, e.g., Elroy-Stein and Moss, Proc. Natl. Acad. Sci. USA (1990) 87:6743-6747; Fuerst et al. Proc. Natl. Acad. Sci. USA (1986) 83:8122-8126.

[0305] Alternatively, avipoxviruses, such as the fowlpox and canarypox viruses, can also be used to deliver the coding sequences of interest. Recombinant avipox viruses, expressing immunogens from mammalian pathogens, are known to confer protective immunity when administered to non-avian species. The use of an Avipox vector is particularly desirable in human and other mammalian species since members of the Avipox genus can only productively replicate in susceptible avian species and therefore are not infective in mammalian cells. Methods for producing recombinant Avipoxviruses are known in the art and employ genetic recombination, as described above with respect to the production of vaccinia viruses. See, e.g., WO 91/12882; WO 89/03429; and WO 92/03545.

[0306] Any of a number of alphavirus vectors can also be used for delivery of polynucleotide compositions of the present invention, such as those vectors described in U.S. Pat. Nos. 5,843,723; 6,015,686; 6,008,035 and 6,015,694. Certain vectors based on Venezuelan Equine Encephalitis (VEE) can also be used, illustrative examples of which can be found in U.S. Pat. Nos. 5,505,947 and 5,643,576.

[0307] Moreover, molecular conjugate vectors, such as the adenovirus chimeric vectors described in Michael et al. J. Biol. Chem. (1993) 268:6866-6869 and Wagner et al. Proc. Natl. Acad. Sci. USA (1992) 89:6099-6103, can also be used for gene delivery under the invention.

[0308] Additional illustrative information on these and other known viral-based delivery systems can be found, for example, in Fisher-Hoch et al., Proc. Natl. Acad. Sci. USA 86:317-321, 1989; Flexner et al., Ann. N.Y. Acad. Sci. 569:86-103, 1989; Flexner et al., Vaccine 8:17-21, 1990; U.S. Pat. Nos. 4,603,112, 4,769,330, and 5,017,487; WO 89/01973; U.S. Pat. No. 4,777,127; GB 2,200,651; EP 0,345,242; WO 91/02805; Berkner, Biotechniques 6:616-627, 1988; Rosenfeld et al., Science 252:431-434, 1991; Kolls et al., Proc. Natl. Acad. Sci. USA 91:215-219, 1994; Kass-Eisler et al., Proc. Natl. Acad. Sci. USA 90:11498-11502, 1993; Guzman et al., Circulation 88:2838-2848, 1993; and Guzman et al., Cir. Res. 73:1202-1207, 1993.

[0309] In certain embodiments, a polynucleotide may be integrated into the genome of a target cell. This integration may be in the specific location and orientation via homologous recombination (gene replacement) or it may be integrated in a random, non-specific location (gene augmentation). In yet further embodiments, the polynucleotide may be stably maintained in the cell as a separate, episomal segment of DNA. Such polynucleotide segments or “episomes” encode sequences sufficient to permit maintenance and replication independent of or in synchronization with the host cell cycle. The manner in which the expression construct is delivered to a cell and where in the cell the polynucleotide remains is dependent on the type of expression construct employed.

[0310] In another embodiment of the invention a polynucleotide is administered/delivered as “naked” DNA, for example as described in Ulmer et al., Science 259:1745-1749, 1993 and reviewed by Cohen, Science 259:1691-1692, 1993. The uptake of naked DNA may be increased by coating the DNA onto biodegradable beads, which are efficiently transported into the cells.

[0311] In still another embodiment, a composition of the present invention can be delivered via a particle bombardment approach, many of which have been described. In one illustrative example, gas-driven particle acceleration can be achieved with devices such as those manufactured by Powderject Pharmaceuticals PLC (Oxford, UK) and Powderject Vaccines Inc. (Madison, Wis.), some examples of which are described in U.S. Pat. Nos. 5,846,796; 6,010,478; 5,865,796; 5,584,807; and EP Pat. No. 0500 799. This approach offers a needle-free delivery approach wherein a dry powder formulation of microscopic particles, such as polynucleotide or polypeptide particles, are accelerated to high speed within a helium gas jet generated by a hand held device, propelling the particles into a target tissue of interest.

[0312] In a related embodiment, other devices and methods that may be useful for gas-driven needle-less injection of compositions of the present invention include those provided by Bioject, Inc. (Portland, Oreg.), some examples of which are described in U.S. Pat. Nos. 4,790,824; 5,064,413; 5,312,335; 5,383,851; 5,399,163; 5,520,639 and 5,993,412.

[0313] According to another embodiment, the pharmaceutical compositions described herein will comprise one or more immunostimulants in addition to the immunogenic polynucleotide, polypeptide, antibody, T-cell and/or APC compositions of this invention. An immunostimulant refers to essentially any substance that enhances or potentiates an immune response (antibody and/or cell-mediated) to an exogenous antigen. One preferred type of immunostimulant comprises an adjuvant. Many adjuvants contain a substance designed to protect the antigen from rapid catabolism, such as aluminum hydroxide or mineral oil, and a stimulator of immune responses, such as lipid A, Bortadella pertussis or Mycobacterium tuberculosis derived proteins. Certain adjuvants are commercially available as, for example, Freund's Incomplete Adjuvant and Complete Adjuvant (Difco Laboratories, Detroit, Mich.); Merck Adjuvant 65 (Merck and Company, Inc., Rahway, N.J.); AS-2 (SmithKline Beecham, Philadelphia, Pa.); aluminum salts such as aluminum hydroxide gel (alum) or aluminum phosphate; salts of calcium, iron or zinc; an insoluble suspension of acylated tyrosine; acylated sugars; cationically or anionically derivatized polysaccharides; polyphosphazenes; biodegradable microspheres; monophosphoryl lipid A and quil A. Cytokines, such as GM-CSF, interleukin-2, -7, -12, and other like growth factors, may also be used as adjuvants.

[0314] Within certain embodiments of the invention, the adjuvant composition is preferably one that induces an immune response predominantly of the Th1 type. High levels of Th1-type cytokines (e.g., IFN-γ, TNFα, IL-2 and IL-12) tend to favor the induction of cell mediated immune responses to an administered antigen. In contrast, high levels of Th2-type cytokines (e.g., IL-4, IL-5, IL-6 and IL-10) tend to favor the induction of humoral immune responses. Following application of a vaccine as provided herein, a patient will support an immune response that includes Th1- and Th2-type responses. Within a preferred embodiment, in which a response is predominantly Th1-type, the level of Th1-type cytokines will increase to a greater extent than the level of Th2-type cytokines. The levels of these cytokines may be readily assessed using standard assays. For a review of the families of cytokines, see Mosmann and Coffman, Ann. Rev. Immunol. 7:145-173, 1989.

[0315] Certain preferred adjuvants for eliciting a predominantly Th1-type response include, for example, a combination of monophosphoryl lipid A, preferably 3-de-O-acylated monophosphoryl lipid A, together with an aluminum salt. MPL® adjuvants are available from Corixa Corporation (Seattle, Wash.; see, for example, U.S. Pat. Nos. 4,436,727; 4,877,611; 4,866,034 and 4,912,094). CpG-containing oligonucleotides (in which the CpG dinucleotide is unmethylated) also induce a predominantly Tk1 response. Such oligonucleotides are well known and are described, for example, in WO 96/02555, WO 99/33488 and U.S. Pat. Nos. 6,008,200 and 5,856,462. Immunostimulatory DNA sequences are also described, for example, by Sato et al., Science 273:352, 1996. Another preferred adjuvant comprises a saponin, such as Quil A, or derivatives thereof, including QS21 and QS7 (Aquila Biopharmaceuticals Inc., Framingham, Mass.); Escin; Digitonin; or Gypsophila or Chenopodium quinoa saponins. Other preferred formulations include more than one saponin in the adjuvant combinations of the present invention, for example combinations of at least two of the following group comprising QS21, QS7, Quil A, β-escin, or digitonin.

[0316] Alternatively the saponin formulations may be combined with vaccine vehicles composed of chitosan or other polycationic polymers, polylactide and polylactide-co-glycolide particles, poly-N-acetyl glucosamine-based polymer matrix, particles composed of polysaccharides or chemically modified polysaccharides, liposomes and lipid-based particles, particles composed of glycerol monoesters, etc. The saponins may also be formulated in the presence of cholesterol to form particulate structures such as liposomes or ISCOMs. Furthermore, the saponins may be formulated together with a polyoxyethylene ether or ester, in either a non-particulate solution or suspension, or in a particulate structure such as a paucilamelar liposome or ISCOM. The saponins may also be formulated with excipients such as Carbopol® to increase viscosity, or may be formulated in a dry powder form with a powder excipient such as lactose.

[0317] In one preferred embodiment, the adjuvant system includes the combination of a monophosphoryl lipid A and a saponin derivative, such as the combination of QS21 and 3D-MPL® adjuvant, as described in WO 94/00153, or a less reactogenic composition where the QS21 is quenched with cholesterol, as described in WO 96/33739. Other preferred formulations comprise an oil-in-water emulsion and tocopherol. Another particularly preferred adjuvant formulation employing QS21, 3D-MPL® adjuvant and tocopherol in an oil-in-water emulsion is described in WO 95/17210.

[0318] Another enhanced adjuvant system involves the combination of a CpG-containing oligonucleotide and a saponin derivative particularly the combination of CpG and QS21 is disclosed in WO 00/09159. Preferably the formulation additionally comprises an oil in water emulsion and tocopherol.

[0319] Additional illustrative adjuvants for use in the pharmaceutical compositions of the invention include Montanide ISA 720 (Seppic, France), SAF (Chiron, Calif., U.S., ISCOMS (CSL), MF-59 (Chiron), the SBAS series of adjuvants (e.g., SBAS-2 or SBAS-4, available from SmithKline Beecham, Rixensart, Belgium), Detox (Enhanzyn®) (Corixa, Hamilton, Mont.), RC-529 (Corixa, Hamilton, Mont.) and other aminoalkyl glucosaminide 4-phosphates (AGPs), such as those described in pending U.S. patent application Ser. Nos. 08/853,826 and 09/074,720, the disclosures of which are incorporated herein by reference in their entireties, and polyoxyethylene ether adjuvants such as those described in WO 99/52549A1.

[0320] Other preferred adjuvants include adjuvant molecules of the general formula

HO(CH₂CH₂O)_(n)—A—R   (I)

[0321] wherein, n is 1-50, A is a bond or —C(O)—, R is C₁₋₅₀ alkyl or Phenyl C₁₋₅₀ alkyl.

[0322] One embodiment of the present invention consists of a vaccine formulation comprising a polyoxyethylene ether of general formula (I), wherein n is between 1 and 50, preferably 4-24, most preferably 9; the R component is C₁₋₅₀, preferably C₄-C₂₀ alkyl and most preferably C₁₂ alkyl, and A is a bond. The concentration of the polyoxyethylene ethers should be in the range 0.1-20%, preferably from 0.1-10%, and most preferably in the range 0.1-1%. Preferred polyoxyethylene ethers are selected from the following group: polyoxyethylene-9-lauryl ether, polyoxyethylene-9-steoryl ether, polyoxyethylene-8-steoryl ether, polyoxyethylene-4-lauryl ether, polyoxyethylene-35-lauryl ether, and polyoxyethylene-23-lauryl ether. Polyoxyethylene ethers such as polyoxyethylene lauryl ether are described in the Merck index (12^(th) edition: entry 7717). These adjuvant molecules are described in WO 99/52549.

[0323] The polyoxyethylene ether according to the general formula (I) above may, if desired, be combined with another adjuvant. For example, a preferred adjuvant combination is preferably with CpG as described in the pending UK patent application GB 9820956.2.

[0324] According to another embodiment of this invention, an immunogenic composition described herein is delivered to a host via antigen presenting cells (APCs), such as dendritic cells, macrophages, B cells, monocytes and other cells that may be engineered to be efficient APCs. Such cells may, but need not, be genetically modified to increase the capacity for presenting the antigen, to improve activation and/or maintenance of the T cell response, to have anti-tumor effects per se and/or to be immunologically compatible with the receiver (i.e., matched HLA haplotype). APCs may generally be isolated from any of a variety of biological fluids and organs, including tumor and peritumoral tissues, and may be autologous, allogeneic, syngeneic or xenogeneic cells.

[0325] Certain preferred embodiments of the present invention use dendritic cells or progenitors thereof as antigen-presenting cells. Dendritic cells are highly potent APCs (Banchereau and Steinman, Nature 392:245-251,1998) and have been shown to be effective as a physiological adjuvant for eliciting prophylactic or therapeutic antitumor immunity (see Timmerman and Levy, Ann. Rev. Med. 50:507-529, 1999). In general, dendritic cells may be identified based on their typical shape (stellate in situ, with marked cytoplasmic processes (dendrites) visible in vitro), their ability to take up, process and present antigens with high efficiency and their ability to activate naive T cell responses. Dendritic cells may, of course, be engineered to express specific cell-surface receptors or ligands that are not commonly found on dendritic cells in vivo or ex vivo, and such modified dendritic cells are contemplated by the present invention. As an alternative to dendritic cells, secreted vesicles antigen-loaded dendritic cells (called exosomes) may be used within a vaccine (see Zitvogel et al.; Nature Med. 4:594-600, 1998).

[0326] Dendritic cells and progenitors may be obtained from peripheral blood, bone marrow, tumor-infiltrating cells, peritumoral tissues-infiltrating cells, lymph nodes, spleen, skin, umbilical cord blood or any other suitable tissue or fluid. For example, dendritic cells may be differentiated ex vivo by adding a combination of cytokines such as GM-CSF, IL-4, IL-13 and/or TNFα to cultures of monocytes harvested from peripheral blood. Alternatively, CD34 positive cells harvested from peripheral blood, umbilical cord blood or bone marrow may be differentiated into dendritic cells by adding to the culture medium combinations of GM-CSF, IL-3, TNFα, CD40 ligand, LPS, flt3 ligand and/or other compound(s) that induce differentiation, maturation and proliferation of dendritic cells.

[0327] Dendritic cells are conveniently categorized as “immature” and “mature” cells, which allows a simple way to discriminate between two well characterized phenotypes. However, this nomenclature should not be construed to exclude all possible intermediate stages of differentiation. Immature dendritic cells are characterized as APC with a high capacity for antigen uptake and processing, which correlates with the high expression of Fcγ receptor and mannose receptor. The mature phenotype is typically characterized by a lower expression of these markers, but a high expression of cell surface molecules responsible for T cell activation such as class I and class II MHC, adhesion molecules (e.g., CD54 and CD11) and costimulatory molecules (e.g., CD40, CD80, CD86 and 4-1BB).

[0328] APCs may generally be transfected with a polynucleotide of the invention (or portion or other variant thereof) such that the encoded polypeptide, or an immunogenic portion thereof, is expressed on the cell surface. Such transfection may take place ex vivo, and a pharmaceutical composition comprising such transfected cells may then be used for therapeutic purposes, as described herein. Alternatively, a gene delivery vehicle that targets a dendritic or other antigen presenting cell may be administered to a patient, resulting in transfection that occurs in vivo. In vivo and ex vivo transfection of dendritic cells, for example, may generally be performed using any methods known in the art, such as those described in WO 97/24447, or the gene gun approach described by Mahvi et al., Immunology and cell Biology 75:456-460, 1997. Antigen loading of dendritic cells may be achieved by incubating dendritic cells or progenitor cells with the tumor polypeptide, DNA (naked or within a plasmid vector) or RNA; or with antigen-expressing recombinant bacterium or viruses (e.g., vaccinia, fowlpox, adenovirus or lentivirus vectors). Prior to loading, the polypeptide may be covalently conjugated to an immunological partner that provides T cell help (e.g., a carrier molecule). Alternatively, a dendritic cell may be pulsed with a non-conjugated immunological partner, separately or in the presence of the polypeptide.

[0329] While any suitable carrier known to those of ordinary skill in the art may be employed in the pharmaceutical compositions of this invention, the type of carrier will typically vary depending on the mode of administration. Compositions of the present invention may be formulated for any appropriate manner of administration, including for example, topical, oral, nasal, mucosal, intravenous, intracranial, intraperitoneal, subcutaneous and intramuscular administration.

[0330] Carriers for use within such pharmaceutical compositions are biocompatible, and may also be biodegradable. In certain embodiments, the formulation preferably provides a relatively constant level of active component release. In other embodiments, however, a more rapid rate of release immediately upon administration may be desired. The formulation of such compositions is well within the level of ordinary skill in the art using known techniques. Illustrative carriers useful in this regard include microparticles of poly(lactide-co-glycolide), polyacrylate, latex, starch, cellulose, dextran and the like. Other illustrative delayed-release carriers include supramolecular biovectors, which comprise a non-liquid hydrophilic core (e.g., a cross-linked polysaccharide or oligosaccharide) and, optionally, an external layer comprising an amphiphilic compound, such as a phospholipid (see e.g., U.S. Pat. No. 5,151,254 and PCT applications WO 94/20078,WO/94/23701 and WO 96/06638). The amount of active compound contained within a sustained release formulation depends upon the site of implantation, the rate and expected duration of release and the nature of the condition to be treated or prevented.

[0331] In another illustrative embodiment, biodegradable microspheres (e.g., polylactate polyglycolate) are employed as carriers for the compositions of this invention. Suitable biodegradable microspheres are disclosed, for example, in U.S. Pat. Nos. 4,897,268; 5,075,109; 5,928,647; 5,811,128; 5,820,883; 5,853,763; 5,814,344, 5,407,609 and 5,942,252. Modified hepatitis B core protein carrier systems such as described in WO/99 40934, and references cited therein, will also be useful for many applications. Another illustrative carrier/delivery system employs a carrier comprising particulate-protein complexes, such as those described in U.S. Pat. No. 5,928,647, which are capable of inducing a class I-restricted cytotoxic T lymphocyte responses in a host.

[0332] The pharmaceutical compositions of the invention will often further comprise one or more buffers (e.g., neutral buffered saline or phosphate buffered saline), carbohydrates (e.g., glucose, mannose, sucrose or dextrans), mannitol, proteins, polypeptides or amino acids such as glycine, antioxidants, bacteriostats, chelating agents such as EDTA or glutathione, adjuvants (e.g., aluminum hydroxide), solutes that render the formulation isotonic, hypotonic or weakly hypertonic with the blood of a recipient, suspending agents, thickening agents and/or preservatives. Alternatively, compositions of the present invention may be formulated as a lyophilizate.

[0333] The pharmaceutical compositions described herein may be presented in unit-dose or multi-dose containers, such as sealed ampoules or vials. Such containers are typically sealed in such a way to preserve the sterility and stability of the formulation until use. In general, formulations may be stored as suspensions, solutions or emulsions in oily or aqueous vehicles. Alternatively, a pharmaceutical composition may be stored in a freeze-dried condition requiring only the addition of a sterile liquid carrier immediately prior to use.

[0334] The development of suitable dosing and treatment regimens for using the particular compositions described herein in a variety of treatment regimens, including e.g., oral, parenteral, intravenous, intranasal, and intramuscular administration and formulation, is well known in the art, some of which are briefly discussed below for general purposes of illustration.

[0335] In certain applications, the pharmaceutical compositions disclosed herein may be delivered via oral administration to an animal. As such, these compositions may be formulated with an inert diluent or with an assimilable edible carrier, or they may be enclosed in hard- or soft-shell gelatin capsule, or they may be compressed into tablets, or they may be incorporated directly with the food of the diet.

[0336] The active compounds may even be incorporated with excipients and used in the form of ingestible tablets, buccal tables, troches, capsules, elixirs, suspensions, syrups, wafers, and the like (see, for example, Mathiowitz et al., Nature Mar. 27, 1997; 386(6623):410-4; Hwang et al., Crit Rev Ther Drug Carrier Syst 1998; 15(3):243-84; U.S. Pat. No. 5,641,515; U.S. Pat. No. 5,580,579 and U.S. Pat. No. 5,792,451). Tablets, troches, pills, capsules and the like may also contain any of a variety of additional components, for example, a binder, such as gum tragacanth, acacia, cornstarch, or gelatin; excipients, such as dicalcium phosphate; a disintegrating agent, such as corn starch, potato starch, alginic acid and the like; a lubricant, such as magnesium stearate; and a sweetening agent, such as sucrose, lactose or saccharin may be added or a flavoring agent, such as peppermint, oil of wintergreen, or cherry flavoring. When the dosage unit form is a capsule, it may contain, in addition to materials of the above type, a liquid carrier. Various other materials may be present as coatings or to otherwise modify the physical form of the dosage unit. For instance, tablets, pills, or capsules may be coated with shellac, sugar, or both. Of course, any material used in preparing any dosage unit form should be pharmaceutically pure and substantially non-toxic in the amounts employed. In addition, the active compounds may be incorporated into sustained-release preparation and formulations.

[0337] Typically, these formulations will contain at least about 0.1% of the active compound or more, although the percentage of the active ingredient(s) may, of course, be varied and may conveniently be between about 1 or 2% and about 60% or 70% or more of the weight or volume of the total formulation. Naturally, the amount of active compound(s) in each therapeutically useful composition may be prepared is such a way that a suitable dosage will be obtained in any given unit dose of the compound. Factors such as solubility, bioavailability, biological half-life, route of administration, product shelf life, as well as other pharmacological considerations will be contemplated by one skilled in the art of preparing such pharmaceutical formulations, and as such, a variety of dosages and treatment regimens may be desirable.

[0338] For oral administration the compositions of the present invention may alternatively be incorporated with one or more excipients in the form of a mouthwash, dentifrice, buccal tablet, oral spray, or sublingual orally-administered formulation. Alternatively, the active ingredient may be incorporated into an oral solution such as one containing sodium borate, glycerin and potassium bicarbonate, or dispersed in a dentifrice, or added in a therapeutically-effective amount to a composition that may include water, binders, abrasives, flavoring agents, foaming agents, and humectants. Alternatively the compositions may be fashioned into a tablet or solution form that may be placed under the tongue or otherwise dissolved in the mouth.

[0339] In certain circumstances it will be desirable to deliver the pharmaceutical compositions disclosed herein parenterally, intravenously, intramuscularly, or even intraperitoneally. Such approaches are well known to the skilled artisan, some of which are further described, for example, in U.S. Pat. No. 5,543,158; U.S. Pat. No. 5,641,515 and U.S. Pat. No. 5,399,363. In certain embodiments, solutions of the active compounds as free base or pharmacologically acceptable salts may be prepared in water suitably mixed with a surfactant, such as hydroxypropylcellulose. Dispersions may also be prepared in glycerol, liquid polyethylene glycols, and mixtures thereof and in oils. Under ordinary conditions of storage and use, these preparations generally will contain a preservative to prevent the growth of microorganisms.

[0340] Illustrative pharmaceutical forms suitable for injectable use include sterile aqueous solutions or dispersions and sterile powders for the extemporaneous preparation of sterile injectable solutions or dispersions (for example, see U.S. Pat. No. 5,466,468). In all cases the form must be sterile and must be fluid to the extent that easy syringability exists. It must be stable under the conditions of manufacture and storage and must be preserved against the contaminating action of microorganisms, such as bacteria and fungi. The carrier can be a solvent or dispersion medium containing, for example, water, ethanol, polyol (e.g., glycerol, propylene glycol, and liquid polyethylene glycol, and the like), suitable mixtures thereof, and/or vegetable oils. Proper fluidity may be maintained, for example, by the use of a coating, such as lecithin, by the maintenance of the required particle size in the case of dispersion and/or by the use of surfactants. The prevention of the action of microorganisms can be facilitated by various antibacterial and antifungal agents, for example, parabens, chlorobutanol, phenol, sorbic acid, thimerosal, and the like. In many cases, it will be preferable to include isotonic agents, for example, sugars or sodium chloride. Prolonged absorption of the injectable compositions can be brought about by the use in the compositions of agents delaying absorption, for example, aluminum monostearate and gelatin.

[0341] In one embodiment, for parenteral administration in an aqueous solution, the solution should be suitably buffered if necessary and the liquid diluent first rendered isotonic with sufficient saline or glucose. These particular aqueous solutions are especially suitable for intravenous, intramuscular, subcutaneous and intraperitoneal administration. In this connection, a sterile aqueous medium that can be employed will be known to those of skill in the art in light of the present disclosure. For example, one dosage may be dissolved in 1 ml of isotonic NaCl solution and either added to 1000 ml of hypodermoclysis fluid or injected at the proposed site of infusion, (see for example, “Remington's Pharmaceutical Sciences” 15th Edition, pages 1035-1038 and 1570-1580). Some variation in dosage will necessarily occur depending on the condition of the subject being treated. Moreover, for human administration, preparations will of course preferably meet sterility, pyrogenicity, and the general safety and purity standards as required by FDA Office of Biologics standards.

[0342] In another embodiment of the invention, the compositions disclosed herein may be formulated in a neutral or salt form. Illustrative pharmaceutically-acceptable salts include the acid addition salts (formed with the free amino groups of the protein) and which are formed with inorganic acids such as, for example, hydrochloric or phosphoric acids, or such organic acids as acetic, oxalic, tartaric, mandelic, and the like. Salts formed with the free carboxyl groups can also be derived from inorganic bases such as, for example, sodium, potassium, ammonium, calcium, or ferric hydroxides, and such organic bases as isopropylamine, trimethylamine, histidine, procaine and the like. Upon formulation, solutions will be administered in a manner compatible with the dosage formulation and in such amount as is therapeutically effective.

[0343] The carriers can further comprise any and all solvents, dispersion media, vehicles, coatings, diluents, antibacterial and antifungal agents, isotonic and absorption delaying agents, buffers, carrier solutions, suspensions, colloids, and the like. The use of such media and agents for pharmaceutical active substances is well known in the art. Except insofar as any conventional media or agent is incompatible with the active ingredient, its use in the therapeutic compositions is contemplated. Supplementary active ingredients can also be incorporated into the compositions. The phrase “pharmaceutically-acceptable” refers to molecular entities and compositions that do not produce an allergic or similar untoward reaction when administered to a human.

[0344] In certain embodiments, the pharmaceutical compositions may be delivered by intranasal sprays, inhalation, and/or other aerosol delivery vehicles. Methods for delivering genes, nucleic acids, and peptide compositions directly to the lungs via nasal aerosol sprays has been described, e.g., in U.S. Pat. No. 5,756,353 and U.S. Pat. No. 5,804,212. Likewise, the delivery of drugs using intranasal microparticle resins (Takenaga et al., J Controlled Release Mar. 2, 1998; 52(1-2):81-7) and lysophosphatidyl-glycerol compounds (U.S. Pat. No. 5,725,871) are also well-known in the pharmaceutical arts. Likewise, illustrative transmucosal drug delivery in the form of a polytetrafluoroetheylene support matrix is described in U.S. Pat. No. 5,780,045.

[0345] In certain embodiments, liposomes, nanocapsules, microparticles, lipid particles, vesicles, and the like, are used for the introduction of the compositions of the present invention into suitable host cells/organisms. In particular, the compositions of the present invention may be formulated for delivery either encapsulated in a lipid particle, a liposome, a vesicle, a nanosphere, or a nanoparticle or the like. Alternatively, compositions of the present invention can be bound, either covalently or non-covalently, to the surface of such carrier vehicles.

[0346] The formation and use of liposome and liposome-like preparations as potential drug carriers is generally known to those of skill in the art (see for example, Lasic, Trends Biotechnol Jul. 16, 1998(7):307-21; Takakura, Nippon Rinsho March 1998; 56(3):691-5; Chandran et al., Indian J Exp Biol. August 1997; 35(8):801-9; Margalit, Crit Rev Ther Drug Carrier Syst. 1995;12(2-3):233-61; U.S. Pat. No. 5,567,434; U.S. Pat. No. 5,552,157; U.S. Pat. No. 5,565,213; U.S. Pat. 5,738,868 and U.S. Pat. No. 5,795,587, each specifically incorporated herein by reference in its entirety).

[0347] Liposomes have been used successfully with a number of cell types that are normally difficult to transfect by other procedures, including T cell suspensions, primary hepatocyte cultures and PC 12 cells (Renneisen et al., J Biol Chem. Sep. 25, 1990; 265(27):16337-42; Muller et al., DNA Cell Biol. April 1990; 9(3):221-9). In addition, liposomes are free of the DNA length constraints that are typical of viral-based delivery systems. Liposomes have been used effectively to introduce genes, various drugs, radiotherapeutic agents, enzymes, viruses, transcription factors, allosteric effectors and the like, into a variety of cultured cell lines and animals. Furthermore, he use of liposomes does not appear to be associated with autoimmune responses or unacceptable toxicity after systemic delivery.

[0348] In certain embodiments, liposomes are formed from phospholipids that are dispersed in an aqueous medium and spontaneously form multilamellar concentric bilayer vesicles (also termed multilamellar vesicles (MLVs).

[0349] Alternatively, in other embodiments, the invention provides for pharmaceutically-acceptable nanocapsule formulations of the compositions of the present invention. Nanocapsules can generally entrap compounds in a stable and reproducible way (see, for example, Quintanar-Guerrero et al., Drug Dev Ind Pharm. December 1998; 24(12):1113-28). To avoid side effects due to intracellular polymeric overloading, such ultrafine particles (sized around 0.1 μm) may be designed using polymers able to be degraded in vivo. Such particles can be made as described, for example, by Couvreur et al., Crit Rev Ther Drug Carrier Syst. 1988;5(1):1-20; zur Muhlen et al., Eur J Pharm Biopharm. March 1998; 45(2):149-55; Zambaux et al. J Controlled Release. Jan 2, 1998; 50(1-3):31-40; and U.S. Pat. No. 5,145,684.

[0350] Cancer Therapeutic Methods

[0351] In further aspects of the present invention, the pharmaceutical compositions described herein may be used for the treatment of cancer, particularly for the immunotherapy of ovarian cancer. Within such methods, the pharmaceutical compositions described herein are administered to a patient, typically a warm-blooded animal, preferably a human. A patient may or may not be afflicted with cancer. Accordingly, the above pharmaceutical compositions may be used to prevent the development of a cancer or to treat a patient afflicted with a cancer. Pharmaceutical compositions and vaccines may be administered either prior to or following surgical removal of primary tumors and/or treatment such as administration of radiotherapy or conventional chemotherapeutic drugs. As discussed above, administration of the pharmaceutical compositions may be by any suitable method, including administration by intravenous, intraperitoneal, intramuscular, subcutaneous, intranasal, intradermal, anal, vaginal, topical and oral routes.

[0352] Within certain embodiments, immunotherapy may be active immunotherapy, in which treatment relies on the in vivo stimulation of the endogenous host immune system to react against tumors with the administration of immune response-modifying agents (such as polypeptides and polynucleotides as provided herein).

[0353] Within other embodiments, immunotherapy may be passive immunotherapy, in which treatment involves the delivery of agents with established tumor-immune reactivity (such as effector cells or antibodies) that can directly or indirectly mediate antitumor effects and does not necessarily depend on an intact host immune system. Examples of effector cells include T cells as discussed above, T lymphocytes (such as CD8⁺ cytotoxic T lymphocytes and CD4⁺ T-helper tumor-infiltrating lymphocytes), killer cells (such as Natural Killer cells and lymphokine-activated killer cells), B cells and antigen-presenting cells (such as dendritic cells and macrophages) expressing a polypeptide provided herein. T cell receptors and antibody receptors specific for the polypeptides recited herein may be cloned, expressed and transferred into other vectors or effector cells for adoptive immunotherapy. The polypeptides provided herein may also be used to generate antibodies or anti-idiotypic antibodies (as described above and in U.S. Pat. No. 4,918,164) for passive immunotherapy.

[0354] Effector cells may generally be obtained in sufficient quantities for adoptive immunotherapy by growth in vitro, as described herein. Culture conditions for expanding single antigen-specific effector cells to several billion in number with retention of antigen recognition in vivo are well known in the art. Such in vitro culture conditions typically use intermittent stimulation with antigen, often in the presence of cytokines (such as IL-2) and non-dividing feeder cells. As noted above, immunoreactive polypeptides as provided herein may be used to rapidly expand antigen-specific T cell cultures in order to generate a sufficient number of cells for immunotherapy. In particular, antigen-presenting cells, such as dendritic, macrophage, monocyte, fibroblast and/or B cells, may be pulsed with immunoreactive polypeptides or transfected with one or more polynucleotides using standard techniques well known in the art. For example, antigen-presenting cells can be transfected with a polynucleotide having a promoter appropriate for increasing expression in a recombinant virus or other expression system. Cultured effector cells for use in therapy must be able to grow and distribute widely, and to survive long term in vivo. Studies have shown that cultured effector cells can be induced to grow in vivo and to survive long term in substantial numbers by repeated stimulation with antigen supplemented with IL-2 (see, for example, Cheever et al., Immunological Reviews 157:177, 1997).

[0355] Alternatively, a vector expressing a polypeptide recited herein may be introduced into antigen presenting cells taken from a patient and clonally propagated ex vivo for transplant back into the same patient. Transfected cells may be reintroduced into the patient using any means known in the art, preferably in sterile form by intravenous, intracavitary, intraperitoneal or intratumor administration.

[0356] Routes and frequency of administration of the therapeutic compositions described herein, as well as dosage, will vary from individual to individual, and may be readily established using standard techniques. In general, the pharmaceutical compositions and vaccines may be administered by injection (e.g., intracutaneous, intramuscular, intravenous or subcutaneous), intranasally (e.g., by aspiration) or orally. Preferably, between 1 and 10 doses may be administered over a 52 week period. Preferably, 6 doses are administered, at intervals of 1 month, and booster vaccinations may be given periodically thereafter. Alternate protocols may be appropriate for individual patients. A suitable dose is an amount of a compound that, when administered as described above, is capable of promoting an anti-tumor immune response, and is at least 10-50% above the basal (i.e., untreated) level. Such response can be monitored by measuring the anti-tumor antibodies in a patient or by vaccine-dependent generation of cytolytic effector cells capable of killing the patient's tumor cells in vitro. Such vaccines should also be capable of causing an immune response that leads to an improved clinical outcome (e.g., more frequent remissions, complete or partial or longer disease-free survival) in vaccinated patients as compared to non-vaccinated patients. In general, for pharmaceutical compositions and vaccines comprising one or more polypeptides, the amount of each polypeptide present in a dose ranges from about 25 μg to 5 mg per kg of host. Suitable dose sizes will vary with the size of the patient, but will typically range from about 0.1 mL to about 5 mL.

[0357] In general, an appropriate dosage and treatment regimen provides the active compound(s) in an amount sufficient to provide therapeutic and/or prophylactic benefit. Such a response can be monitored by establishing an improved clinical outcome (e.g., more frequent remissions, complete or partial, or longer disease-free survival) in treated patients as compared to non-treated patients. Increases in preexisting immune responses to a tumor protein generally correlate with an improved clinical outcome. Such immune responses may generally be evaluated using standard proliferation, cytotoxicity or cytokine assays, which may be performed using samples obtained from a patient before and after treatment.

[0358] Cancer Detection and Diagnostic Compositions, Methods and Kits

[0359] In general, a cancer may be detected in a patient based on the presence of one or more ovarian tumor proteins and/or polynucleotides encoding such proteins in a biological sample (for example, blood, sera, sputum urine and/or tumor biopsies) obtained from the patient. In other words, such proteins may be used as markers to indicate the presence or absence of a cancer such as ovarian cancer. In addition, such proteins may be useful for the detection of other cancers. The binding agents provided herein generally permit detection of the level of antigen that binds to the agent in the biological sample. Polynucleotide primers and probes may be used to detect the level of mRNA encoding an ovarian tumor protein, which is also indicative of the presence or absence of a cancer. In general, a ovarian tumor sequence should be present at a level that is at least three fold higher in tumor tissue than in normal tissue

[0360] There are a variety of assay formats known to those of ordinary skill in the art for using a binding agent to detect polypeptide markers in a sample. See, e.g., Harlow and Lane, Antibodies: A Laboratory Manual, Cold Spring Harbor Laboratory, 1988. In general, the presence or absence of a cancer in a patient may. be determined by (a) contacting a biological sample obtained from a patient with a binding agent; (b) detecting in the sample a level of polypeptide that binds to the binding agent; and (c) comparing the level of polypeptide with a predetermined cut-off value.

[0361] In a preferred embodiment, the assay involves the use of binding agent immobilized on a solid support to bind to and remove the polypeptide from the remainder of the sample. The bound polypeptide may then be detected using a detection reagent that contains a reporter group and specifically binds to the binding agent/polypeptide complex. Such detection reagents may comprise, for example, a binding agent that specifically binds to the polypeptide or an antibody or other agent that specifically binds to the binding agent, such as an anti-immunoglobulin, protein G, protein A or a lectin. Alternatively, a competitive assay may be utilized, in which a polypeptide is labeled with a reporter group and allowed to bind to the immobilized binding agent after incubation of the binding agent with the sample. The extent to which components of the sample inhibit the binding of the labeled polypeptide to the binding agent is indicative of the reactivity of the sample with the immobilized binding agent. Suitable polypeptides for use within such assays include full length ovarian tumor proteins and polypeptide portions thereof to which the binding agent binds, as described above.

[0362] The solid support may be any material known to those of ordinary skill in the art to which the tumor protein may be attached. For example, the solid support may be a test well in a microtiter plate or a nitrocellulose or other suitable membrane. Alternatively, the support may be a bead or disc, such as glass, fiberglass, latex or a plastic material such as polystyrene or polyvinylchloride. The support may also be a magnetic particle or a fiber optic sensor, such as those disclosed, for example, in U.S. Pat. No. 5,359,681. The binding agent may be immobilized on the solid support using a variety of techniques known to those of skill in the art, which are amply described in the patent and scientific literature. In the context of the present invention, the term “immobilization” refers to both noncovalent association, such as adsorption, and covalent attachment (which may be a direct linkage between the agent and functional groups on the support or may be a linkage by way of a cross-linking agent). Immobilization by adsorption to a well in a microtiter plate or to a membrane is preferred. In such cases, adsorption may be achieved by contacting the binding agent, in a suitable buffer, with the solid support for a suitable amount of time. The contact time varies with temperature, but is typically between about 1 hour and about 1 day. In general, contacting a well of a plastic microtiter plate (such as polystyrene or polyvinylchloride) with an amount of binding agent ranging from about 10 ng to about 10 μg, and preferably about 100 ng to about 1 μg, is sufficient to immobilize an adequate amount of binding agent.

[0363] Covalent attachment of binding agent to a solid support may generally be achieved by first reacting the support with a bifunctional reagent that will react with both the support and a functional group, such as a hydroxyl or amino group, on the binding agent. For example, the binding agent may be covalently attached to supports having an appropriate polymer coating using benzoquinone or by condensation of an aldehyde group on the support with an amine and an active hydrogen on the binding partner (see, e.g., Pierce Immunotechnology Catalog and Handbook, 1991, at A12-A13).

[0364] In certain embodiments, the assay is a two-antibody sandwich assay. This assay may be performed by first contacting an antibody that has been immobilized on a solid support, commonly the well of a microtiter plate, with the sample, such that polypeptides within the sample are allowed to bind to the immobilized antibody. Unbound sample is then removed from the immobilized polypeptide-antibody complexes and a detection reagent (preferably a second antibody capable of binding to a different site on the polypeptide) containing a reporter group is added. The amount of detection reagent that remains bound to the solid support is then determined using a method appropriate for the specific reporter group.

[0365] More specifically, once the antibody is immobilized on the support as described above, the remaining protein binding sites on the support are typically blocked. Any suitable blocking agent known to those of ordinary skill in the art, such as bovine serum albumin or Tween 20™ (Sigma Chemical Co., St. Louis, Mo.). The immobilized antibody is then incubated with the sample, and polypeptide is allowed to bind to the antibody. The sample may be diluted with a suitable diluent, such as phosphate-buffered saline (PBS) prior to incubation. In general, an appropriate contact time (i.e., incubation time) is a period of time that is sufficient to detect the presence of polypeptide within a sample obtained from an individual with ovarian cancer. Preferably, the contact time is sufficient to achieve a level of binding that is at least about 95% of that achieved at equilibrium between bound and unbound polypeptide. Those of ordinary skill in the art will recognize that the time necessary to achieve equilibrium may be readily determined by assaying the level of binding that occurs over a period of time. At room temperature, an incubation time of about 30 minutes is generally sufficient.

[0366] Unbound sample may then be removed by washing the solid support with an appropriate buffer, such as PBS containing 0.1% Tween 20™. The second antibody, which contains a reporter group, may then be added to the solid support. Preferred reporter groups include those groups recited above.

[0367] The detection reagent is then incubated with the immobilized antibody-polypeptide complex for an amount of time sufficient to detect the bound polypeptide. An appropriate amount of time may generally be determined by assaying the level of binding that occurs over a period of time. Unbound detection reagent is then removed and bound detection reagent is detected using the reporter group. The method employed for detecting the reporter group depends upon the nature of the reporter group. For radioactive groups, scintillation counting or autoradiographic methods are generally appropriate. Spectroscopic methods may be used to detect dyes, luminescent groups and fluorescent groups. Biotin may be detected using avidin, coupled to a different reporter group (commonly a radioactive or fluorescent group or an enzyme). Enzyme reporter groups may generally be detected by the addition of substrate (generally for a specific period of time), followed by spectroscopic or other analysis of the reaction products.

[0368] To determine the presence or absence of a cancer, such as ovarian cancer, the signal detected from the reporter group that remains bound to the solid support is generally compared to a signal that corresponds to a predetermined cut-off value. In one preferred embodiment, the cut-off value for the detection of a cancer is the average mean signal obtained when the immobilized antibody is incubated with samples from patients without the cancer. In general, a sample generating a signal that is three standard deviations above the predetermined cut-off value is considered positive for the cancer. In an alternate preferred embodiment, the cut-off value is determined using a Receiver Operator Curve, according to the method of Sackett et al., Clinical Epidemiology: A Basic Science for Clinical Medicine, Little Brown and Co., 1985, p. 106-7. Briefly, in this embodiment, the cut-off value may be determined from a plot of pairs of true positive rates (i.e., sensitivity) and false positive rates (100%-specificity) that correspond to each possible cut-off value for the diagnostic test result. The cut-off value on the plot that is the closest to the upper left-hand corner (i.e., the value that encloses the largest area) is the most accurate cut-off value, and a sample generating a signal that is higher than the cut-off value determined by this method may be considered positive. Alternatively, the cut-off value may be shifted to the left along the plot, to minimize the false positive rate, or to the right, to minimize the false negative rate. In general, a sample generating a signal that is higher than the cut-off value determined by this method is considered positive for a cancer.

[0369] In a related embodiment, the assay is performed in a flow-through or strip test format, wherein the binding agent is immobilized on a membrane, such as nitrocellulose. In the flow-through test, polypeptides within the sample bind to the immobilized binding agent as the sample passes through the membrane. A second, labeled binding agent then binds to the binding agent-polypeptide complex as a solution containing the second binding agent flows through the membrane. The detection of bound second binding agent may then be performed as described above. In the strip test format, one end of the membrane to which binding agent is bound is immersed in a solution containing the sample. The sample migrates along the membrane through a region containing second binding agent and to the area of immobilized binding agent. Concentration of second binding agent at the area of immobilized antibody indicates the presence of a cancer. Typically, the concentration of second binding agent at that site generates a pattern, such as a line, that can be read visually. The absence of such a pattern indicates a negative result. In general, the amount of binding agent immobilized on the membrane is selected to generate a visually discernible pattern when the biological sample contains a level of polypeptide that would be sufficient to generate a positive signal in the two-antibody sandwich assay, in the format discussed above. Preferred binding agents for use in such assays are antibodies and antigen-binding fragments thereof. Preferably, the amount of antibody immobilized on the membrane ranges from about 25 ng to about 1 μg, and more preferably from about 50 ng to about 500 ng. Such tests can typically be performed with a very small amount of biological sample.

[0370] Of course, numerous other assay protocols exist that are suitable for use with the tumor proteins or binding agents of the present invention. The above descriptions are intended to be exemplary only. For example, it will be apparent to those of ordinary skill in the art that the above protocols may be readily modified to use tumor polypeptides to detect antibodies that bind to such polypeptides in a biological sample. The detection of such tumor protein specific antibodies may correlate with the presence of a cancer.

[0371] A cancer may also, or alternatively, be detected based on the presence of T cells that specifically react with a tumor protein in a biological sample. Within certain methods, a biological sample comprising CD4⁺ and/or CD8⁺ T cells isolated from a patient is incubated with a tumor polypeptide, a polynucleotide encoding such a polypeptide and/or an APC that expresses at least an immunogenic portion of such a polypeptide, and the presence or absence of specific activation of the T cells is detected. Suitable biological samples include, but are not limited to, isolated T cells. For example, T cells may be isolated from a patient by routine techniques (such as by Ficoll/Hypaque density gradient centrifugation of peripheral blood lymphocytes). T cells may be incubated in vitro for 2-9 days (typically 4 days) at 37° C. with polypeptide (e.g., 5-25 μg/ml). It may be desirable to incubate another aliquot of a T cell sample in the absence of tumor polypeptide to serve as a control. For CD4⁺ T cells, activation is preferably detected by evaluating proliferation of the T cells. For CD8⁺ T cells, activation is preferably detected by evaluating cytolytic activity. A level of proliferation that is at least two fold greater and/or a level of cytolytic activity that is at least 20% greater than in disease-free patients indicates the presence of a cancer in the patient.

[0372] As noted above, a cancer may also, or alternatively, be detected based on the level of mRNA encoding a tumor protein in a biological sample. For example, at least two oligonucleotide primers may be employed in a polymerase chain reaction (PCR) based assay to amplify a portion of a tumor cDNA derived from a biological sample, wherein at least one of the oligonucleotide primers is specific for (i.e., hybridizes to) a polynucleotide encoding the tumor protein. The amplified cDNA is then separated and detected using techniques well known in the art, such as gel electrophoresis. Similarly, oligonucleotide probes that specifically hybridize to a polynucleotide encoding a tumor protein may be used in a hybridization assay to detect the presence of polynucleotide encoding the tumor protein in a biological sample.

[0373] To permit hybridization under assay conditions, oligonucleotide primers and probes should comprise an oligonucleotide sequence that has at least about 60%, preferably at least about 75% and more preferably at least about 90%, identity to a portion of a polynucleotide encoding a tumor protein of the invention that is at least 10 nucleotides, and preferably at least 20 nucleotides, in length. Preferably, oligonucleotide primers and/or probes hybridize to a polynucleotide encoding a polypeptide described herein under moderately stringent conditions, as defined above. Oligonucleotide primers and/or probes which may be usefully employed in the diagnostic methods described herein preferably are at least 10-40 nucleotides in length. In a preferred embodiment, the oligonucleotide primers comprise at least 10 contiguous nucleotides, more preferably at least 15 contiguous nucleotides, of a DNA molecule having a sequence as disclosed herein. Techniques for both PCR based assays and hybridization assays are well known in the art (see, for example, Mullis et al., Cold Spring Harbor Symp. Quant Biol., 51:263, 1987; Erlich ed., PCR Technology, Stockton Press, NY, 1989).

[0374] One preferred assay employs RT-PCR, in which PCR is applied in conjunction with reverse transcription. Typically, RNA is extracted from a biological sample, such as biopsy tissue, and is reverse transcribed to produce cDNA molecules. PCR amplification using at least one specific primer generates a cDNA molecule, which may be separated and visualized using, for example, gel electrophoresis. Amplification may be performed on biological samples taken from a test patient and from an individual who is not afflicted with a cancer. The amplification reaction may be performed on several dilutions of cDNA spanning two orders of magnitude. A two-fold or greater increase in expression in several dilutions of the test patient sample as compared to the same dilutions of the non-cancerous sample is typically considered positive.

[0375] In another embodiment, the compositions described herein may be used as markers for the progression of cancer. In this embodiment, assays as described above for the diagnosis of a cancer may be performed over time, and the change in the level of reactive polypeptide(s) or polynucleotide(s) evaluated. For example, the assays may be performed every 24-72 hours for a period of 6 months to 1 year, and thereafter performed as needed. In general, a cancer is progressing in those patients in whom the level of polypeptide or polynucleotide detected increases over time. In contrast, the cancer is not progressing when the level of reactive polypeptide or polynucleotide either remains constant or decreases with time.

[0376] Certain in vivo diagnostic assays may be performed directly on a tumor. One such assay involves contacting tumor cells with a binding agent. The bound binding agent may then be detected directly or indirectly via a reporter group. Such binding agents may also be used in histological applications. Alternatively, polynucleotide probes may be used within such applications.

[0377] As noted above, to improve sensitivity, multiple tumor protein markers may be assayed within a given sample. It will be apparent that binding agents specific for different proteins provided herein may be combined within a single assay. Further, multiple primers or probes may be used concurrently. The selection of tumor protein markers may be based on routine experiments to determine combinations that results in optimal sensitivity. In addition, or alternatively, assays for tumor proteins provided herein may be combined with assays for other known tumor antigens.

[0378] The present invention further provides kits for use within any of the above diagnostic methods. Such kits typically comprise two or more components necessary for performing a diagnostic assay. Components may be compounds, reagents, containers and/or equipment. For example, one container within a kit may contain a monoclonal antibody or fragment thereof that specifically binds to a tumor protein. Such antibodies or fragments may be provided attached to a support material, as described above. One or more additional containers may enclose elements, such as reagents or buffers, to be used in the assay. Such kits may also, or alternatively, contain a detection reagent as described above that contains a reporter group suitable for direct or indirect detection of antibody binding.

[0379] Alternatively, a kit may be designed to detect the level of mRNA encoding a tumor protein in a biological sample. Such kits generally comprise at least one oligonucleotide probe or primer, as described above, that hybridizes to a polynucleotide encoding a tumor protein. Such an oligonucleotide may be used, for example, within a PCR or hybridization assay. Additional components that may be present within such kits include a second oligonucleotide and/or a diagnostic reagent or container to facilitate the detection of a polynucleotide encoding a tumor protein.

[0380] The following Examples are offered by way of illustration and not by way of limitation.

EXAMPLES Example 1 Identification of Representative Ovarian Carcinoma cDNA Sequences

[0381] Primary ovarian tumor and metastatic ovarian tumor cDNA libraries were each constructed in kanamycin resistant pZErO™-2 vector (Invitrogen) from pools of three different ovarian tumor RNA samples. For the primary ovarian tumor library, the following RNA samples were used: (1) a moderately differentiated papillary serous carcinoma of a 41 year old, (2) a stage IIIC ovarian tumor and (3) a papillary serous adenocarcinoma for a 50 year old Caucasian. For the metastatic ovarian tumor library, the RNA samples used were omentum tissue from: (1) a metastatic poorly differentiated papillary adenocarcinoma with psammoma bodies in a 73 year old, (2) a metastatic poorly differentiated adenocarcinoma in a 74 year old and (3) a metastatic poorly differentiated papillary adenocarcinoma in a 68 year old.

[0382] The number of clones in each library was estimated by plating serial dilutions of unamplified libraries. Insert data were determined from 32 primary ovarian tumor clones and 32 metastatic ovarian tumor clones. The library characterization results are shown in Table II. TABLE II CHARACTERIZATION OF cDNA LIBRARIES # Clones Clones with Insert Size Ave. Insert Library in Library Insert (%) Range (bp) Size (bp) Primary Ovarian 1,258,000  97 175-8000 2356 Tumor Metastatic 1,788,000 100 150-4300 1755 Ovarian Tumor

[0383] Four subtraction libraries were constructed in ampicillin resistant pcDNA3.1 vector (Invitrogen). Two of the libraries were from primary ovarian tumors and two were from metastic ovarian tumors. In each case, the number of restriction enzyme cuts within inserts was minimized to generate full length subtraction libraries. The subtractions were each done with slightly different protocols, as described in more detail below.

[0384] A. POTS 2 Library: Primary Ovarian Tumor Subtraction Library Tracer: 10 μg primary ovarian tumor library, digested with Not I Driver: 35 μg normal pancreas in pcDNA3.1(+) 20 μg normal PBMC in pcDNA3.1(+) 10 μg normal skin in pcDNA3.1(+) 35 μg normal bone marrow in pZErO ™-2 Digested with Bam HI/Xho I/Sca I

[0385] Two hybridizations were performed, and Not I-cut pcDNA3.1(+) was the cloning vector for the subtracted library. Sequence results for previously unidentified clones that were randomly picked from the subtracted library are presented in Table III. *TABLE III OVARIAN CARCINOMA SEQUENCES Sequence SEQ ID NO 21907 1 21909 2 21911 5 21920 9 21921 10 25099 143 25101 144 25103 145 25107 146 25111 148 25113 149 25115 150 25116 151 25752 156 25757 158 25763 160 25769 161 25770 162

[0386] B. POTS 7 Library: Primary Ovarian Tumor Subtraction Library Tracer:   10 μg primary ovarian tumor library, digested with Not I Driver   35 μg normal pancreas in pcDNA3.1(+)   20 μg normal PBMC in pcDNA3.1(+)   10 μg normal skin in pcDNA3.1(+)   35 μg normal bone marrow in pZErO ™-2 Digested with Bam HI/Xho I/Sca I ˜25 μg pZErO ™-2, digested with Bam HI and Xho I

[0387] Two hybridizations were performed, and Not I-cut pcDNA3.1(+) was the cloning vector for the subtracted library. Sequence results for previously unidentified clones that were randomly picked from the subtracted library are presented in Table IV. TABLE IV OVARIAN CARCINOMA SEQUENCES Sequence SEQ ID NO 24937 125 24940 128 24946 132 24950 133 24951 134 24955 136 24956 137 25791 166 25796 167 25797 168 25804 171

[0388] C. OS1D Library: Metastic Ovarian Tumor Subtraction Library Tracer:   10 μg metastatic ovarian library in pZErO ™-2, digested with Not I Driver: 24.5 μg normal pancreas in pcDNA3.1   14 μg normal PBMC in pcDNA3.1   14 μg normal skin in pcDNA3.1 24.5 μg normal bone marrow in pZErO ™-2   50 μg pZErO ™-2, digested with Bam HI/Xho I/Sfu I

[0389] Three hybridizations were performed, and the last two hybridizations were done with an additional 15 μg of biotinylated pZErO™-2 to remove contaminating pZErO™-2 vectors. The cloning vector for the subtracted library was pcDNA3.1/Not I cut. Sequence results for previously unidentified clones that were randomly picked from the subtracted library are presented in Table V. TABLE V Ovarian Carcinoma Sequences Sequence SEQ ID NO 23645.1 13 23660.1 16 23666.1 19 23679.1 23 24635 57 24647 63 24651 65 24661 69 24663 70 24664 71 24670 72 24675 75 24683 78

[0390] D. OS1F Library: Metastatic Ovarian Tumor Subtraction Library Tracer:   10 μg metastatic ovarian tumor library, digested with Not I Driver: 12.8 μg normal pancreas in pcDNA3.1  7.3 μg normal PBMC in pcDNA3.1  7.3 μg normal skin in pcDNA3.1 12.8 μg normal bone marrow in pZErO ™-2   25 μg pZErO ™-2, digested with Bam HI/Xho I/Sfu I

[0391] One hybridization was performed. The cloning vector for the subtracted library was pcDNA3.1/Not I cut. Sequence results for previously unidentified clones that were randomly picked from the subtracted library are presented in Table VI. TABLE VI OVARIAN CARCINOMA SEQUENCES Sequence SEQ ID NO 24336 (79% with H. sapiens mitochondrial 27       genome (consensus sequence)) 24337 28 24341 (91% Homo sapiens chromosome 5, 32       BAC clone 249h5 (LBNL H149) 24344 33 24348 35 24351 38 24355 (91% Homo sapiens chromosome 17, 41       clone hCIT.91_J_4) 24356 42 24357 (87% S. scrofa mRNA for UDP glu- 43       cose pyrophosphorylase) 24358 44 24359 (78% Human mRNA for KIAA0111 45       gene, complete cds) 24360 46 24361 47 24362 (88% Homo sapiens Chromosome 16 48       BAC clone CIT987SK-A-233A7) 24363 (87% Homo sapiens eukaryotic 49       translation elongation factor 1       alpha 1 (EEF1A1) 24364 (89% Human DNA sequence from PAC 50       27K14 on chromosome Xp11.3-Xp11.4) 24367 (89% Homo sapiens 12p13.3 BAC 52       RCPI11-935C2) 24368 53 24690 81 24692 82 24694 84 24696 86 24699 89 24701 90 24703 91 24704 (88% Homo sapiens chromosome 9, 92       clone hRPK.401_G_18) 24705 93 24707 95 24709 97 24711 98 24713 99 24714 (91% Human DNA sequence from clone 100       125N5 on chromosome 6q26-27) 24717 (89% Homo sapiens proliferation- 103       associated gene A (natural       killer-enhancing factor A) (PAGA) 24727 107 24732 111 24737 (84% Human ADP/ATP translocase 114       mRNA) 24741 117 24745 120 24746 121

[0392] The sequences in Table VII, which correspond to known sequences, were also identified in the above libraries. TABLE VII OVARIAN CARCINOMA SEQUENCES SEQ ID Identity NO Sequence Library H. sapiens DNA for muscle nicotinic 3 21910 POTS2 acetylcholine receptor gene promotor, clone ICRFc105F02104 Homo sapiens complement component 3 (C3) 4 21913 POTS2 gene, exons 1-30. Homo sapiens SWI/SNF related, matrix 6 21914 POTS2 associated, actin dependent regulator of chromatin, subfamily a, member 4 (SMARCA4) Human ferritin Heavy subunit mRNA, complete 7 21915 POTS2 cds. Homo sapiens CGI-151 protein mRNA, 8 21916 POTS2 complete cds Human BAC clone GS055K18 from 7p15-p21 11 23636.1 OS1D HUMGFIBPA Human growth hormone- 12 23637.1 OS1D dependent insulin-like growth factor-binding protein Homo sapiens ribosomal protein, large, PO 14 23647.1 OS1D (RPLPO) mRNA HUMTRPM2A Human TRPM-2 mRNA 15 23657.1 OS1D HUMMTA Homo sapiens mitochondrial DNA 17 23661.1 OS1D HSU78095 Homo sapiens placental bikunin 18 23662.1 OS1D mRNA HUMTI227HC Human mRNA for TI-227H 20 23669.1 OS1D HUMMTCG Human mitochondrion 21 23673.1 OS1D Homo sapiens FK506-binding protein 1A 22 23677.1 OS1D (12kD) (FKBP1A) mRNA Homo sapiens mRNA for zinc-finger DNA- 24 24333 OS1F binding protein, complete cds Homo sapiens mRNA; cDNA DKFZp564E1962 25 24334 OS1F (from clone DKFZp564E1962) Homo sapiens tumor protein, translationally- 26 24335 OS1F controlled 1 (TPT1) mRNA. Homo sapiens interleukin 1 receptor accessory 29 24338 OS1F protein (IL1RAP) mRNA. Human mRNA for KIAA0026 gene 30 24339 OS1F Homo sapiens K-Cl cotransporter KCC4 31 24340 OS1F mRNA, complete cds Homo sapiens nuclear chloride ion channel 34 24345 OS1F protein (NCC27) mRNA Homo sapiens mRNA for DEPP (decidual 36 24349 OS1F protein induced by progesterone) Homo sapiens atrophin-1 interacting protein 4 37 24350 OS1F (AIP4) mRNA Human collagenase type IV mRNA, 3′ end. 39 24352 OS1F Human mRNA for T-cell cyclophilin 40 24354 OS1F Homo sapiens tumor suppressing 51 24366 OS1F subtransferable candidate 1 (TSSC1) Homo sapiens clone 24452 mRNA sequence 54 24374 OS1F Homo sapiens eukaryotic translation 55 24627 OS1D elongation factor 1 alpha 1 (EEF1A1) Genomic sequenc efrom Human 9q34 56 24634 OS1D Human insulin-like growth factor-binding 58 24636 OS1D protein-3 gene Human ribosomal protein L3 mRNA, 3′ end 59 24638 OS1D Homo sapiens annexin II (lipocortin II) (ANX2) 60 24640 OS1D mRNA Homo sapiens tubulin, alpha, ubiquitous (K- 61 24642 OS1D ALPHA-1) Human non-histone chromosomal protein 62 24645 OS1D HMG-14 mRNA Homo sapiens ferritin, heavy polypeptide 1 64 24648 OS1D (FTH1) Homo sapiens 12p13.3 PAC RPCI1-96H9 66 24653 OS1D (Roswell Park Cancer Institute Human) PACLibrary) Homo sapiens T cell-specific tyrosine kinase 67 24655 OS1D mRNA Homo sapiens keratin 18 (KRT18) mRNA 68 24657 OS1D Homo sapiens growth arrest specific transcript 73 24671 OS1D 5 gene Homo sapiens ribosomal protein S7 (RPS7) 74 24673 OS1D Homo sapiens mRNA; cDNA DKFZp564H182 76 24677 OS1D Human TSC-22 protein mRNA 77 24679 OS1D Human mRNA for ribosomal protein 79 24687 OS1D Genomic sequence from Human 13 80 24689 OS1F Homo sapiens clone IMAGE 286356 83 24693 OS1F Homo sapiens v-fos FBJ murine osteosarcoma 85 24695 OS1F viral oncogene homolog(FOS) mRNA Homo sapiens hypothetical 43.2 Kd protein 87 24697 OS1F mRNA Human heat shock protein 27 (HSPB1) gene 88 24698 OS1F exons 1-3 Homo sapiens senescence-associated 94 24706 OS1F epithelial membrane protein (SEMP1) Human ferritin H chain mRNA 96 24708 OS1F Homo sapiens mRNA for KIAA0287 gene 101 24715 OS1F Homo sapiens CGI-08 protein mRNA 102 24716 OS1F H. sapiens CpG island DNA genomic Mse1 104 24719 OS1F fragment, clone 84a5 Human clone 23722 mRNA 105 24721 OS1F Homo sapiens zinc finger protein slug (SLUG) 106 24722 OS1F gene Homo sapiens (clone L6) E-cadherin (CDH1) 108 24728 OS1F gene Homo sapiens ribosomal protein L13 (RPL13) 109 24729 OS1F H. sapiens RNA for snRNP protein B 110 24730 OS1F Homo sapiens mRNA; cDNA DKFZp434K114 112 24734 OS1F Homo sapiens cornichon protein mRNA 113 24735 OS1F Homo sapiens keratin 8 (KRT8) mRNA 115 24739 OS1F Human DNA sequence from PAC 29K1 on 116 24740 OS1F chromosome 6p21.3-22.2. Homo sapiens mRNA for KIAA0762 protein 118 24742 OS1F Human clones 23667 and 23775 zinc finger 119 24744 OS1F protein mRNA Human H19 RNA gene, complete cds. 122 24933 POTS7 Human triosephosphate isomerase mRNA, 123 24934 POTS7 complete cds. Human cyclooxygenase-1 (PTSG1) mRNA, 124 24935 POTS7 partial cds Homo sapiens megakaryocyte potentiating 126 24938 POTS7 factor (MPF) mRNA. Human mRNA for Apo1_Human (MER5(Aop1- 127 24939 POTS7 Mouse)-like protein), complete cds Homo sapiens arylacetamide deacetylase 129 24942 POTS7 (esterase) (AADAC) mRNA. Homo sapiens echinoderm microtubule- 130 24943 POTS7 associated protein-like EMAP2 mRNA, complete cds Homo sapiens podocalyxin-like (PODXL) 131 24944 POTS7 mRNA. Homo sapiens synaptogyrin 2 (SYNGR2) 135 24952 POTS7 mRNA. Homo sapiens amyloid beta precursor protein- 138 24959 POTS7 binding protein 1, 59kD (APPBP1) mRNA. Human aldose reductase mRNA, complete 139 24969 POTS7 cds. Genomic sequence from Human 9q34, 140 25092 POTS2 complete sequence [Homo sapiens] Human glyceraldehyde-3-phosphate 141 25093 POTS2 dehydrogenase (GAPDH) mRNA, complete cds. Homo sapiens breast cancer suppressor 142 25098 POTS2 candidate 1 (bcsc-1) mRNA, complete cds Homo sapiens SKB1 (S. cerevisiae) homolog 147 25110 POTS2 (SKB1) mRNA. Homo sapiens prepro dipeptidyl peptidase I 152 25117 POTS2 (DPP-I) gene, complete cds Homo sapiens preferentially expressed antigen 153 25745 POTS2 of melanoma (PRAME) mRNA Human translocated t(8;14) c-myc (MYC) 154 25746 POTS2 oncogene, exon 3 and complete cds Human 12S RNA induced by poly(rI), poly(rC) 155 25749 POTS2 and Newcastle disease virus Human mRNA for fibronectin (FN precursor) 157 25755 POTS2 Homo sapiens mRNA for hepatocyte growth 159 25758 POTS2 factor activator inhibitor type 2, complete cds Homo sapiens mRNA for KIAA0552 protein, 163 25771 POTS7 complete cds Homo sapiens IMP (inosine monophosphate) 164 25775 POTS7 dehydrogenase 2 (IMPDH2) mRNA Homo sapiens clone 23942 alpha enolase 165 25787 POTS7 mRNA, partial cds H. sapiens vegf gene, 3′ UTR 169 25799 POTS7 Homo sapiens 30S ribosomal protein S7 170 25802 POTS7 homolog mRNA, complete cds Homo sapiens acetyl-Coenzyme A 172 25808 POTS7 acetyltransferase 2 (acetoacetyl Coenzyme A thiolase) (ACAT2) mRNA Homo sapiens Norrie disease protein (NDP) 173 25809 POTS7 mRNA

[0393] Still further ovarian carcinoma polynucleotide and/or polypeptide sequences identified from the above libraries are provided below in Table VIII. Sequences O574S (SEQ ID NO:183 & 185), O584S (SEQ ID NO:193) and O585S (SEQ ID NO:194) represent novel sequences. The remaining sequences exhibited at least some homology with known genomic and/or EST sequences. TABLE VIII SEQ ID: Sequence Library 174: O565S_CRABP OS1D 175: O566S_Ceruloplasmin POTS2 176: O567S_41191.SEQ(1 > 487) POTS2 177: O568S_KIAA0762.seq(1 > 3999) POTS7 178: O569S_41220.seq(1 > 1069) POTS7 179: O570S_41215.seq(1 > 1817) POTS2 180: O571S_41213.seq(1 > 2382) POTS2 181: O572S_41208.seq(1 > 2377) POTS2 182: O573S_41177.seq(1 > 1370) OS1F 183: O574S_47807.seq(1 > 2060) n/a 184: O568S/VSGF DNA seq n/a 185: O574S_47807.seq(1 > 3000) n/a 186: O568S/VSGF protein seq n/a 187: 449H1(57581) OS1D 188: 451E12(57582) OS1D 189: 453C7_3′(57583.1)Osteonectin OS1D 190: 453C7_5′(57583.2) OS1D 191: 456G1_3′(57584.1)Neurotensin OS1F 192: 456G1_5′(57584.2) OS1F 193: O584S_465G5(57585) OS1F 194: O585S_469B12(57586) POTS2 195: O569S_474C3(57587) POTS7 196: 483B1_3′(24934.1)Triosephosphate POTS7 197: 57885 Human preferentially expressed POTS2 antigen of melanoma 198: 57886 Chromosome 22q12.1 clone CTA- POTS2 723E4 199: 57887 Homologous to mouse brain cDNA POTS2 clone MNCb-0671

[0394] Further studies on the clone of SEQ ID NO:182 (also referred to as O573S) led to the identification of multiple open reading frames that encode the amino acid sequences of SEQ ID NO:200-202.

Example 2 Analysis of cDNA Expression Using Microarray Technology

[0395] In additional studies, sequences disclosed herein were found to be overexpressed in specific tumor tissues as determined by microarray analysis. Using this approach, cDNA sequences are PCR amplified and their mRNA expression profiles in tumor and normal tissues are examined using cDNA microarray technology essentially as described (Shena et al., 1995). In brief, the clones are arrayed onto glass slides as multiple replicas, with each location corresponding to a unique cDNA clone (as many as 5500 clones can be arrayed on a single slide or chip). Each chip is hybridized with a pair of cDNA probes that are fluorescence-labeled with Cy3 and Cy5 respectively. Typically, 1 μg of polyA⁺ RNA is used to generate each cDNA probe. After hybridization, the chips are scanned and the fluorescence intensity recorded for both Cy3 and Cy5 channels. There are multiple built-in quality control steps. First, the probe quality is monitored using a panel of ubiquitously expressed genes. Secondly, the control plate also can include yeast DNA fragments of which complementary RNA may be spiked into the probe synthesis for measuring the quality of the probe and the sensitivity of the analysis. Currently, the technology offers a sensitivity of 1 in 100,000 copies of mRNA. Finally. the reproducibility of this technology can be ensured by including duplicated control cDNA elements at different locations.

[0396] The microarray results for clones 57885 (SEQ ID NO:197), 57886 (SEQ ID NO:198) and 57887 (SEQ ID NO:199) are as follows.

[0397] Clone 57885: 16/38 (42%) of ovarian tumors showed an expression signal value of >0.4. The mean value for all ovary tumors was 0.662 with a mean value of 0.187 for all normal tissues, which yields a 3.64 fold overexpression level in ovary tumor relative to essential normal tissues. Normal tissue expression was elevated (>0.4) in peritoneum, skin and thymus.

[0398] Clone 57886: 16/38 (42%) of ovarian tumors showed an expression signal value of >0.4. The mean value for all ovary tumors was 0.574 with a mean value of 0.166 for all normal tissues which yields a 3.46 fold overexpression level in ovary tumor relative to essential normal tissues. Normal tissue expression was elevated (>0.4) in heart, pancreas and small intestive.

[0399] Clone 57887: 17/38 (44%) of ovarian tumors showed an expression signal value of >0.4. The mean value for all ovary tumors is 0.744 with a mean value of 0.184 for all normal tissues which yields a 4.04 fold overexpression level in ovary tumor relative to essential normal tissues. Normal tissue expression was elevated (>0.4) in esophagus.

Example 3 Expression of Recombinant Antigen O568S in E. Coli

[0400] This example describes the expression of recombinant antigen O568S (SEQ ID NO:177) in E. coli. This sequence was identified in Example 1 from the POTS 7 subtraction library using primary ovarian tumor cDNA as the tracer. PCR primers specific for the open reading frame of O568S were designed and used in the specific amplification of O568S. The PCR product was enzymatically digested with EcoRI and ligated into pPDM, a modified pET28 vector which had been cut with the restriction enzymes EcoRI and Eco721. The construct sequence and orientation was confirmed through sequence analysis, the sequence of which is shown in SEQ ID NO:206. The vector was then transformed into the expression hosts, BLR (DE3) and HMS 174 (DE3) pLys S. Protein expression was confirmed, the sequence of which is provided in SEQ ID NO:207.

Example 4 Additional Sequence Obtained for Clone O591 S

[0401] The sequence of O591S (clone identifier 57887) was used to search public sequence databases. It was found that the reverse strand showed some degree of identity to the C-terminal end of GPR39. The cDNA for the coding region of GPR39 is disclosed in SEQ ID NO:208 and the corresponding amino acid sequence in SEQ ID NO:209. The GPR39 coding region contains two exons. Both O591S and GPR39, encoded by the complementary strand of O591S, are located on chromosome 2.

Example 5 Further Characterization of O591S and Identification of Extended Sequence

[0402] O1034C is an ovary specific gene identified by electronic subtraction. Briefly, electronic subtraction involves an analysis of EST database sequences to identify ovarian-specific genes. In the electronic subtraction method used to identify O1034C, sequences of EST clones derived from ovary libraries (normal and tumor) were obtained from the GenBank public human EST database. Each ovary sequence was used as a “seed” query in a BLASTN search of the total human EST database to identify other EST clones that share sequence with the seed sequence (clones that potentially originated from the same mRNA). EST clones with shared sequence were grouped into clusters, and clusters that shared sequence with other clusters were grouped into superclusters. The tissue source of each EST within each supercluster was noted, and superclusters were ranked based on the distribution of the tissues from which the ESTs originated. Superclusters that comprise primarily, or solely, EST clones from ovary libraries were considered to represent genes that were differentially expressed in ovary tissue, relative to all other normal adult tissue.

[0403] This clone was identified from the public EST databases as Integrated Molecular Analysis of Genomics and their Expression (IMAGE) clone number 595449 (the IMAGE consortium is a repository of EST clones and cDNA clones) and is disclosed as SEQ ID NO:210. Accession numbers AA173739 and AA173383 represents the sequence of the identified EST in Genebank. This clone is part of Unigene cluster HS.85339 (Unigene is an experimental system for automatically partitioning Genbank sequences into a non-redundant set of gene-orientated clusters) and was annotated as encoding a neurotensin-like G protein coupled receptor (GRP39). However, the inventors have discovered that IMAGE#595449 encodes a novel protein derived from the complementary strand to that which encodes the potential GPR39.

[0404] Microarray analysis of the clone using a series of ovary tumor specific probes indicated that this clone was over expressed 4.95-fold in a group of ovary tumor and normal ovary samples as compared to a group of essential normal tissue samples.

[0405] IMAGE#59449 was subjected to a Blast A search of the EST database and Genbank and an electronic full length clone contig (01034C) was generated by extending IMAGE#595449 and its resulting contigs to completion. This process was repeated to completion when no further EST sequences were identified to extend the consensus sequence. This electronically derived clone was identified as coding a previously described clone, O591S, the sequence of which is disclosed in SEQ ID NO:211. The discovery of this ovary specific candidate is described in more detail in Example 4.

[0406] The consensus sequence for O1034C extended further 5′ than O591S due to the additional sequences derived from two EST clones, accession numbers BF345141 and BE336607, the sequences for which are disclosed in SEQ ID NO:212 and 213 respectively. Although BF345141 diverges from the O1034C/O591S consensus at its 3′-end (possibly representing a different splice form), and from BE336607 at several bases at its 5′-end, the two ESTs were compared to the available matching chromosome sequence. They were found on human chromosome 2, clone RP11-159N20:htgs database accession number AC010974. These sequences were used to extend 01034C/O591S to form a final consensus sequence for O1034C/O591S of 1897 base pairs, disclosed in SEQ ID NO:214.

[0407] An open reading frame (ORF) was identified within the O1034C/O591S consensus sequence (nucleotides 260-682), the predicted translation of which is disclosed in SEQ ID NO:215. A BLASTx database search against the Genbank database indicated that this ORF had no identity (E value <1e-25) with any known human protein. The only match was with the G protein-coupled receptors, including GPR39, which the inventors have shown to be encoded at the 3′-end of O1034C/O591S on the complementary strand. However, the ORF did encode a protein that had 93% similarity (131/141 amino acids) and 91% identity (129/141 amino acids) with an un-named murine product (Accession #BAA95101), suggesting that this is a real translation product that represents a novel human ovary-specific antigen.

[0408] The novelty of O1034C/O591S was confirmed by Northern Blot analysis using single stranded probes that complement either GRP39 or O1034C/O591S. The strand-specific O1034C/O591S probe specifically hybridized to the ovary tumor samples probed on the Northern blot, whilst all samples were negative when probed with GPR39. In addition real-time PCR was performed using primers specific for either GPR39 or O1034C/O591S. These results further demonstrated the differential expression profiles of the two sequences. This protein is a putative membrane protein as determined from Corixa's Tmpred protein prediction algorithm.

Example 6 Expression Analysis and Further Characterization of Ovarian Sequence O568S

[0409] The ovarian sequence O568S was originally identified as cDNA clone 24742 (SEQ ID NO:1 18). Using clone 24742 as a query sequence to search public sequence databases, the sequence was found to have a high degree of homology with KIAA0762 (SEQ ID NO:177) and with VSGF. The DNA sequence for VSGF is provided in SEQ ID 184 and the VSGF protein sequence is provided in SEQ ID NO:186.

[0410] Real-time PCR (see Gibson et al., Genome Research 6:995-1001, 1996; Heid et al., Genome Research 6:986-994, 1996) is a technique that evaluates the level of PCR product accumulation during amplification. This technique permits quantitative evaluation of mRNA levels in multiple samples. Briefly, mRNA is extracted from tumor and normal tissue and cDNA is prepared using standard techniques. Real-time PCR is performed, for example, using a Perkin Elmer/Applied Biosystems (Foster City, Calif.) 7700 Prism instrument. Matching primers and fluorescent probes are designed for genes of interest using, for example, the primer express program provided by Perkin Elmer/Applied Biosystems (Foster City, Calif.). Optimal concentrations of primers and probes are initially determined by those of ordinary skill in the art, and control (e.g., β-actin) primers and probes are obtained commercially from, for example, Perkin Elmer/Applied Biosystems (Foster City, Calif.). To quantitate the amount of specific RNA in a sample, a standard curve is generated using a plasmid containing the gene of interest. Standard curves are generated using the Ct values determined in the real-time PCR, which are related to the initial cDNA concentration used in the assay. Standard dilutions ranging from 10-10⁶ copies of the gene of interest are generally sufficient. In addition, a standard curve is generated for the control sequence. This permits standardization of initial RNA content of a tissue sample to the amount of control for comparison purposes.

[0411] By RealTime PCR analysis, O568 was highly overexpressed in the majority of ovary tumors and ovary tumor metastases tested relative to normal ovary tissue and relative to an extensive normal tissue panel. Little or no expression was observed in normal esophagus, spinal cord, bladder, colon, liver, PBMC (activated or resting), lung, skin, small intestine, stomach, skeletal muscle, pancreas, dendritic cells, heart, spleen bone marrow, thyroid, trachea, thymus, bronchia, cerebellum, ureter, uterus and peritoneum epithelium. Some low level expression was observed in normal breast, brain, bone, kidney, adrenal gland and salivary gland, but the expression levels in these normal tissues were generally at least several fold less than the levels observed in ovary tumors overexpressing O568S.

[0412] Moreover, a series of Northern blots was performed which also demonstrated that the ORF region of O568S is specifically overexpressed in ovary tumors. The initial blot contained RNA from a series of normal tissues as well as from ovary tumors. This blot was probed using, as a labeled probe, DNA from O568S that corresponded to the 3′UTR of the VSGF sequence disclosed in SEQ ID NO:184. This blot revealed an ovary tumor-specific 5.0 Kb message as well as a potential 3.5 Kb brain specific message and a ubiquitously expressed 1.35 Kb message.

[0413] Another Northern blot was performed with RNAs from a number of different brain tissues and probed with the 3′UTR region as above. Five of eleven brain samples showed overexpression of the 3.5 Kb message. In order to determine whether the ORF region of O568S was specifically overexpressed in ovary tumors, a series of three blots was carried out using three separate probes designed from within the VSGF ORF of O568S. Results from these experiments clearly indicated that only the 5.0 Kb message is expressed in ovary tumor.

Example 7 Synthesis of Polypeptides

[0414] Polypeptides are synthesized on a Perkin Elmer/Applied Biosystems Division 430A peptide synthesizer using FMOC chemistry with HPTU (O-Benzotriazole-N,N,N′,N′-tetramethyluronium hexafluorophosphate) activation. A Gly-Cys-Gly sequence is attached to the amino terminus of the peptide to provide a method of conjugation, binding to an immobilized surface, or labeling of the peptide. Cleavage of the peptides from the solid support is carried out using the following cleavage mixture: trifluoroacetic acid:ethanedithiol:thioanisole:water:phenol (40:1:2:2:3). After cleaving for 2 hours, the peptides are precipitated in cold methyl-t-butyl-ether. The peptide pellets are then dissolved in water containing 0.1% trifluoroacetic acid (TFA) and lyophilized prior to purification by C18 reverse phase HPLC. A gradient of 0%-60% acetonitrile (containing 0.1% TFA) in water (containing 0.1% TFA) is used to elute the peptides. Following lyophilization of the pure fractions, the peptides are characterized using electrospray or other types of mass spectrometry and by amino acid analysis.

Example 8 O568S Northern Blot Analysis

[0415] As described in Example 6, Northern blot analysis demonstrated that the ORF region of O568S was specifically over expressed in ovarian tumors. The original probe used corresponded to the 3′UTR of the VSGF sequence disclosed in SEQ ID NO:184. The results from these Northern blots revealed an ovarian tumor-specific 5.0 Kb message as well as a potential 3.5 Kb brain specific message. To confirm that the entire region covered by the ORF yields a single 5.0 Kb ovarian tumor-specific message two additional probes were designed. The probes were located at the 5′ and 3′ regions of the ORF. Northern blot analysis using these two probes demonstrated that both probes hybridized to a 5.0 Kb product present only in ovarian tumor samples. Both probes failed to hybridize with RNA derived from multiple brain samples.

Example 9 Real Time PCR and Northern Blot Analysis of O590S

[0416] Real time PCR analysis of ovarian tumor antigen O590S was performed essentially as described in Example 6. O590S specific primers and probe were designed and quantitative Real Time PCR was performed on a panel of cDNAs prepared from a variety of tissues including ovarian tumor samples and a panel of normal tissues. This analysis revealed that O590S-specific mRNA was over expressed in approximately 65% of ovarian tumor samples tested, 100% tumor samples derived from SCID mice, and 100% ovarian tumor cell lines tested, when compared to normal ovarian tissue. No detectable expression was observed in normal tissues.

[0417] In addition to Real Time PCR, Northern blot analysis was performed to determine to transcript size of O590S. The Northern blot was probed with a 537 bp PCR product specific for O590S, which was designed to avoid regions of repeat sequences. This probe revealed a smeared band that was approximately 9.0 Kb in size, which was present in the majority of ovarian tumor samples tested.

Example 10 Analysis of cDNA Expression Using Microarray Technology

[0418] This example describes microarray expression analysis of ovary tumor- and tissue-specific cDNAs identified from OTCLS4, POTS2 and POTS7 (Subtraction libraries described in Example 1). Microarray analysis was performed essentially as described in Example 2. Sequence expression was determined by probing with a number of ovarian tumor samples, including papillary serous cystic carcinoma, papillary serous adenocarcinoma, papillary serous neoplasm, papillary serous carcinoma, papillary serous cytstadenocarcinoma, and a panel of normal tissues including adrenal gland, pituitary gland, thymus, bronchus, stomach, pancreas, skin, spinal cord, kidney, spleen, brain, breast, small intestine, thyroid, trachea, colon, PBMC resting, PBMC activated, lung, aorta, bone marrow, mammary epithelial tissue, esophagus, heart, and liver.

[0419] Clones showing an ovarian tumor mean or median value that was at least two fold greater than the normal tissue value were selected for further analysis. Further selection criteria was imposed on mean and median values as follows:

[0420] Mean tumor value≧0.2 and mean normal value of<0.4

[0421] Median tumor value≧0.2 and median normal value of<0.3.

[0422] Based on the selection criteria above, 26 clones were selected from the OTCLS4, POTS2 and POTS7 for sequencing. These sequences are disclosed herein in SEQ ID NOS:216-243. See Table IX for details. TABLE IX SEQ ID GenBank Ratio NO Clone ID ID NO GenBank Description Ratio 1/2 Group 1 Group 2 216 91226.5 15779016 Homo sapiens, clone IMAGE:4047062, mRNA Mean 2.09 0.722 0.346 217 91227.2 14760620 Homo sapiens bHLH protein DEC2 (DEC2), Mean 2.45 0.62 0.153 mRNA 218 91230.2 13543043 Homo sapiens, hypothetical protein dJ473B4, Mean 2.17 0.434 0.2 clone MGC:4987 IMAGE:3450155, mRNA, complete cds 219 91231 13277551 Homo sapiens, coxsackie virus and adenovirus Mean 2.16 0.545 0.253 receptor, clone MGC:5086 IMAGE:3463613, mRNA, complete cds 220 91238.3 12804424 Homo sapiens, similar to phosphoserine Mean 2.18 0.229 0.105 aminotransferase, clone MGC:1460 IMAGE:3544564, mRNA, complete cds 221 91239.6 14589888 Homo sapiens cadherin 2, type 1, N-cadherin Median 2.22 0.581 0.262 (neuronal) (CDH2), mRNA 222 91240.2 5729900 Homo sapiens IGF-II mRNA-binding protein 3 Mean 2.08 0.236 0.114 (KOC1), mRNA 223 91241.2 12653176 Homo sapiens, MAD2 (mitotic arrest deficient, Median 2.13 0.316 0.148 yeast, homolog)-like 1, clone MGC:8662 IMAGE:2964388, mRNA, complete cds 224 91242.5 12653176 Homo sapiens, MAD2 (mitotic arrest deficient, Mean 2.36 0.458 0.194 yeast, homolog)-like 1, clone MGC:8662 IMAGE:2964388, mRNA, complete cds 225 91243.6 15297244 Homo sapiens laminin, gamma 2 (nicein Mean 2.91 0.755 0.26 (100kD), kalinin (105kD), BM600 (100kD), Herlitz junctional epidermolysis bullosa)) (LAMC2), mRNA 226 91245.2 7022574 Homo sapiens cDNA FLJ 10500 fis, clone Mean 2.1 0.571 0.272 NT2RP2000369 227 91246.4 1575533 Human MAD2 (hsMAD2) mRNA, complete cds Median 2.51 0.292 0.116 228 91247.3 5912166 Homo sapiens mRNA; cDNA DKFZp564H1663 Mean 2.03 0.369 0.182 (from clone DKFZp564H1663) 229 91247.4 5912166 Homo sapiens mRNA; cDNA DKFZp564H1663 Mean 2.03 0.369 0.182 (from clone DKFZp564H1663) 230 91249.2 14711935 Homo sapiens, hypothetical protein FLJ10461, Mean 2.26 0.271 0.12 clone IMAGE:4102110, mRNA 231 91253.2 14756011 Homo sapiens similar to coxsackie virus and Mean 2.4 0.411 0.172 adenovirus receptor; 46kD coxsackie and adenovirus receptor (CAR) protein (H. sapiens) (LOC93529), mRNA 232 91254.2 11493240 Human DNA sequence from clone RP11- Mean 5.15 1.396 0.271 124N19 on chromosome 13, complete sequence [Homo sapiens] 233 91259.2 14771329 Homo sapiens Wilms tumor (WT1), mRNA Mean 3.87 0.406 0.105 234 91261.3 11465000 Homo sapiens 12 BAC RP11-283G6 (Roswell Mean 2.57 0.34 0.132 Park Cancer Institute Human BAC library) complete sequence 235 91261.4 11465000 Homo sapiens 12 BAC RP11-283G6 (Roswell Mean 2.57 0.34 0.132 Park Cancer Institute Human BAC library) complete sequence 236 91262.2 4506070 Homo sapiens protein kinase C, iota (PRKC1), Mean 2.46 0.695 0.282 mRNA 237 91263.2 13647850 Homo sapiens matrix metalloproteinase 11 Mean 2.63 0.254 0.097 (stromolysin 3) (MMP11), mRNA 238 91264.2 NA NOVEL (no GENSEQ) Mean 15.6 2.058 0.132 239 91268.2 3980529 Homo sapiens PAC clone RP4-797C5 from Mean 2.41 0.232 0.096 7q31, complete sequence 240 91269.5 NA NOVEL (no GENSEQ) Mean 3.04 0.226 0.074 241 91271.5 339440 Homo sapiens transcriptional enhancer factor Mean 2.1 0.407 0.194 (TEF1) DNA, complete cds 242 91273.3 15297244 Homo sapiens laminin, gamma 2 (nicein Mean 2.5 0.625 0.25 (100kD), kalinin (105kD), BM600 (100kD), Herlitz junctional epidermolysis bullosa)) (LAMC2), mRNA 243 91274.6 NA NOVEL (GENSEQ″AAQ60336) Mean 2.58 0.204 0.079

Example 11 Expression Analysis and Further Characterization of Ovarian Sequence O646S

[0423] Ovarian tumor antigen O646S was originally described in Example 10 as clone 91274.6 (SEQ ID NO:243). Using SEQ ID NO:243 to search publicly available databases, a contig was generated, the DNA sequence of which is disclosed in SEQ ID NO:246, with a corresponding protein sequence disclosed in SEQ ID NO:249. This sequence was shown to share homology with Genbank Accession Number 18549403, the DNA and protein sequences of which are disclosed in SEQ ID NOS:244 and 247, respectively, and Genbank Accession Number FLJ14035, the DNA and protein sequences for which are disclosed in SEQ ID NOS:245 and 248, respectively.

Example 12 Further Characterization of Ovarian Sequence O648S

[0424] Ovarian tumor antigen O648S was originally described in Example 10 as clone 91268.2 (SEQ ID NO:239). Using SEQ ID NO:239 to search publicly available databases, a contig was generated, the DNA sequence of which is disclosed in SEQ ID NO:256, with a corresponding protein sequence disclosed in SEQ ID NO:261. This sequence was shown to share homology with several sequences including, Genbank Accession Number 3980529, the DNA sequence of which is disclosed in SEQ ID NOS:250, Genbank Accession Number 13629915, the DNA and protein sequences for which are disclosed in SEQ ID NOS:251 and 257, Genbank Accession Number 9789986, the DNA and protein sequences of which are disclosed in SEQ ID NOS:252 and 258, respectively, Genbank Accession Number 6006516, the DNA and protein sequences of which are disclosed in SEQ ID NOS:253 and 259, Genbank Accession Number 5689424, the DNA and protein sequences of which are disclosed in SEQ ID NOS:254 and 260, and Genbank Accession Number 15638833 the DNA sequence of which is disclosed in SEQ ID NO:255.

Example 13 Further Characterization of Ovarian Sequence O647S

[0425] Ovarian tumor antigen O647S was originally described in Example 10 as clone 91261.3 (SEQ ID NO:234). Using SEQ ID NO:234 to search publicly available databases, a contig was generated, the DNA sequence of which is disclosed in SEQ ID NO:268. This sequence was shown to share homology with several sequences, including Genbank Accession Number 16933560, the DNA and protein sequences of which are disclosed in SEQ ID NOS:262 and 269, Genbank Accession Number 12053028, the DNA and protein sequences for which are disclosed in SEQ ID NOS:263 and 270, Genbank Accession Number 7638812, the DNA and protein sequences of which are disclosed in SEQ ID NOS:264 and 271, Genbank Accession Number 939922, the DNA and protein sequences of which are disclosed in SEQ ID NOS:265 and 272, Genbank Accession Number 6093230, the DNA sequence of which are disclosed in SEQ ID NO:266 and Genbank Accession Number 11465000, the DNA sequence of which is disclosed in SEQ ID NO:267.

Example 14 Further Characterization of Ovarian Sequence O648S

[0426] Ovarian tumor antigen 0645S was originally described in Example 10 as clone 91264.2 (SEQ ID NO:238). Using SEQ ID NO:238 to search publicly available databases, a contig was generated, the DNA sequence of which is disclosed in SEQ ID NO:273.

Example 15 Further Characterization of Ovarian Sequence O644S

[0427] Ovarian tumor antigen O644S was originally described in Example 10 as clone 91269.5 (SEQ ID NO:240). Using SEQ ID NO:240 to search publicly available databases, a contig was generated, the DNA sequence of which is disclosed in SEQ ID NO:277. This sequence was found to contain three open reading frames, the sequences of which are disclosed in SEQ ID NOS:280-282. These sequences were shown to share homology with Genbank Accession Number NM006580, the DNA and protein sequences of which are disclosed in SEQ ID NOS:274 and 278, Genbank Accession Number AF152101.1, the DNA and protein sequences for which are disclosed in SEQ ID NOS:275 and 279, and Genbank Accession Number 18425237, the DNA sequence of which is disclosed in SEQ ID NOS:276.

Example 16 O591S Expression in E. Coli

[0428] The identification and characterization of O591S (SEQ ID NO: 214, encoding the protein of SEQ ID NO: 215) was described above (Example 1 and 4). For production and purification of O591S protein used for antibody generation, a truncated form of O591S, lacking the signal peptide sequence, was expressed in E. coli using a modified pET 28 vector with an N-terminal histidine tag.

[0429] The truncated coding region of O591 S-A was PCR amplified minus the signal sequence (amino acids 24-141) with the following primer pairs: CBH-005 (SEQ ID NO:287) 5′ cacttcttgcttccaggctttgcgctgcaaat 3′ CBH-003 (SEQ ID NO:288) 5′ actagctcgagtcagcagtgtgccgagaa 3′

[0430] PCR amplification was performed under the following reaction conditions:

[0431] 10 μl 10×Pfu buffer

[0432] 1 μl 10 mM dNTPs

[0433] 2 μl 10 μM of each primer

[0434] 83 μl of sterile water

[0435] 1.5 μl Pfu DNA polymerase (Stratagene, La Jolla, Calif.)

[0436] 50 ηg DNA

[0437] The reaction was amplified under the following conditions:

[0438] 96° C. 2 minutes, followed by 40 cycles of

[0439] 96° C. 20 seconds, 64° C. 15 seconds, and 72° C. 1 minute,

[0440] With a final extension step of 72° C. for 4 minutes.

[0441] The PCR product was digested with Xho I and cloned into pPDM His (a modified pET28 vector with a histidine tag in frame on the 5′ end) that has been digested with Eco721 and XhoI. Constructs were confirmed through nucleic acid sequence analysis, the corresponding DNA and protein sequence for which are disclosed in SEQ ID NOS:283 and 284, respectively. Following sequence analysis, the construct was then transformed into BLR (DE3) pLys S and HMS 174 (DE3) pLys S cells.

Example 17 The Generation of Rabbit Anti-O568S Polyclonal Antibodies and Expression Determination in Ovarian Tumors

[0442] The over-expression of O568S in ovarian tumor samples and normal ovary was verified using affinity purified rabbit polyclonal antibodies to O568S in the immunohistorchemical (IHC) analysis of ovarian tumors and normal tissues.

[0443] Rabbits were immunized with purified recombinant O568S protein and polyclonal antibodies prepared. Briefly, production and purification of the O568S antigen used for antibody generation was as follows:

[0444] The ovarian tumor protein antigen O568S (amino acids 29-808) was expressed in an E. coli recombinant expression system and grown overnight at 37° C. in LB Broth with the appropriate antibiotics in a shaking incubator. The next morning, 10 ml of the overnight culture was added to 500 ml of 2× YT plus the appropriate antibiotics in a 2L-baffled Erlenmeyer flask. When the Optical Density (at 560 nanometers) of the culture reached 0.4-0.6 the cells were induced with IPTG (1 mM) for 4 hours, and then harvested by centrifugation, washed with phosphate buffered saline and centrifuged again. The supernatant was discarded and the cells were either processed immediately or frozen for future use. When processed immediately, in order to break open the E. coli cells, twenty milliliters of lysis buffer was added to the cell pellets, followed by vortex mixing and French Press disruption at a pressure of 16,000 psi. This lysed cell suspension was then centrifuged, the resulting supernatant and pellet fractions of which were examined by SDS-PAGE for the presence of recombinant protein.

[0445] The pellet prepared as described above was resuspended in 10 mM Tris pH 8.0, 1% CHAPS, washed and centrifuged again. This step was repeated an additional two times. The washed pellet containing inclusion bodies was then solubilized with either 8 M urea or 6 M guanidine HCl containing 10 mM Tris pH 8.0 plus 10 mM imidazole (solubilization buffer). The solubilized protein was added to 5 ml of nickel-chelate resin (Qiagen Inc.) and incubated for 45 min to 1 hour at room temperature with continuous agitation. After incubation, the resin and protein mixture was added to a disposable column and the flow through containing unbound proteins was collected. The column containing resin with bound protein was then washed with 10-20 column volumes of solubilization buffer, and eluted using an elution buffer solution containing 8M urea, 10 mM tris pH 8.0 and 300 mM imidazole. Column fractions (amounting to 3 ml of elution buffer each) were collected and examined by SDS-PAGE for the presence of O568S protein. Fractions containing the desired protein were pooled for further characterization. As an additional purification step, a strong anion exchange resin such as Hi-Prep Q (Biorad) was equilibrated with the appropriate buffer and the pooled fractions containing O568S protein were loaded onto this column and eluted using an increasing salt gradient. Fractions were collected and again evaluated by SDS-PAGE for the presence of O568S protein. The appropriate fractions were identified, combined and dialyzed against 10 mM Tris pH 8.0. Purity was determined by SDS-PAGE or HPLC, the concentration of purified protein was determined by Lowry assay or Amino Acid Analysis, the amino terminal protein sequence was determined to confirm authenticity, and the level of endotoxin was determined using a standard Limulus (LAL) assay. Fractions containing purified O568S were pooled, sterilized by filtration using a 0.22 micron filter, aliquoted and frozen until needed.

[0446] For the generation of polyclonal antiserum, rabbits were immunized with 400 micrograms of purified O568S protein combined with 100 micrograms of muramyldipeptide (MDP) and an equal volume of Incomplete Freund's Adjuvant (IFA). Every four weeks thereafter, animals were boosted with 100 micrograms of O568S antigen mixed with an equal volume of IFA. Seven days following each boost a blood sample from each immunized animal was taken and a serum fraction therefrom prepared by incubating the blood sample at 4° C. for 12-24 hours, clarified by centrifugation.

[0447] In order to characterize the above-mentioned rabbit polyclonal anti-O568S antiserum, 96 well plates were coated with the appropriate antigen in 50 μl (typically 1 μg of protein), incubated at 4C. for 20 hours, after which 250 μl of BSA blocking buffer was added followed by an additional 2 hours of incubation at room temperature (RT). Each well was then washed 6 times with PBS/0.01% tween. The rabbit anti-O568S antiserum to be tested was diluted in PBS, 50 μl of which was added to each well and incubated at RT for 30 minutes. Plates were washed as described above and then 50 μl of a 1:10000 dilution of goat anti-rabbit horse radish peroxidase (HRP) conjugated antibody was added and incubated at RT for 30 minutes. Next plates were washed as described above and 100 μl of TMB containing microwell Peroxidase was added. Substrate was added to each well, incubated for 15 minutes in the dark at RT, the calorimetric reaction stopped with the addition of 100 μl of 1 N H2SO4 and signal determined immediately at 450 nm.

[0448] For IHC analysis, paraffin embedded formalin-fixed tissue was sliced into 4 micron sections. Steam heat induced epitope retrieval (SHIER) in 0.1M sodium citrate buffer (pH 6.0) was used for optimal staining conditions. Sections were incubated with 10% serum/PBS for 5 minutes. Primary antibody (0.5 μg/ml rabbit affinity purified anti-O568S polyclonal antibody) was added to each section for 25 minutes at varying concentrations, followed by a 25 minute incubation with an anti-rabbit biotinylated antibody. Rabbit IgG was also tested on all tissues and served as a negative control. Endogenous peroxidase activity was blocked by three 1.5 minute incubations with hydrogen peroxidase. The avidin biotin complex/horse radish peroxidase (ABC/HRP) system was used along with DAB chromogen to visualize antigen expression. Slides were counterstained with hematoxylin.

[0449] The tissues tested and their expression profiles are described in detail in Table X. Of the ovarian cancer metastases tested, six were adenocarcinomas, five of which tested positive and one was marginal. The majority of the tumor samples stained positive with a strong membrane localized signal, demonstrating that O568S is expressed on the surface of the tumor cells. TABLE X Tissue Expression of O568S TISSUE O568S EXPRESSION Ovarian cancer 3/5 Ovarian cancer metastases  8/12 Normal ovary 3/4 Normal lung (alveolar epithelium) 0/1 Normal lung (bronchiole epithelium) 0/1 Brain (cortex) 6/6 (marginal staining of selected neuronal populations) Brain (spinal cord) 6/6 (marginal staining of purkinje cells) Stomach 5/5 (marginal staining of selected neuronal populations) Skin 0/1 Heart 0/1 Kidney 0/1 Liver 0/1 Colon 0/1 Tonsil 0/1 Vagina 1/1 (squamous epithelium)

Example 18 Real-Time PCR Analysis of Ovarian Tumor Antigens Identified from the OTCLS4, POTS2 and POTS7 Libraries

[0450] Clones identified as having a good expression profile by microarray analysis (as described in Example 10), were further analyzed by real-time PCR on an extended panel of ovarian tumor and normal tissue samples (including ovary, aorta, adrenal gland, bladder, bone, bronchus, brain, breast, CD34+ cells, dendritic cells, esophagus, heart, kidney, large intestine, liver, lung, lymph nodes, pancreas, peritoneum, bane marrow, skin, small intestine, spinal cord, spleen, stomach, thymus, thyroid, tonsil, trachea, ureter, uterus). Real time PCR was performed as described above in Example 6.

[0451] The first-strand cDNA used in the quantitative real-time PCR was synthesized from 20 μg of total RNA that was treated with DNase I (Amplification Grade, Gibco BRL Life Technology, Gaithersburg, Md.), using Superscript Reverse Transcriptase (RT) (Gibco BRL). Real-time PCR was performed with an ABIPRISM 7900 sequence detection system (PE Biosystems, Foster City, Calif.). The 7900 system uses SYBR™ green, a fluorescent dye that only intercalates into double stranded DNA, and a set of gene-specific forward and reverse primers. The increase in fluorescence was monitored during the whole amplification process. The optimal concentration of primers was determined using a checkerboard approach, and a pool of cDNAs from tumors was used in this process. The PCR reaction was performed in 12.5 μl volumes that included 2.5 μl of SYBR green buffer, 2 μl of cDNA template and 2.5 μl each of the forward and reverse primers for the gene of interest. The cDNAs used for RT reactions were diluted 1:10 for each gene of interest and 1:100 for the β-actin control. The expression of the gene of interest in various tissue samples was represented by comparative C_(T) (threshold cycle) method. C_(T) indicates the fractional cycle number at which the amount of amplified target reaches a fixed threshold. The C_(T) value of normal aorta, skin, peritoneum, thyroid gland, dendritic cells, or CD34⁺ cells was used as a comparative reference in order to evaluate the over-expression levels seen with each of the genes.

[0452] The following clones have been evaluated on the extended ovarian real-time panel. In some cases where expression was fairly ubiquitous, mean real-time expression values were determined for ovarian tumor (not including ovarian tumor cell line and SCID samples), normal ovarian, and other normal tissues (not including normal ovary). All clones were found to be over-expressed in ovarian tumor to some degree, demonstrating their use as tumor immunotherapeutics and/or diagnostic targets.

[0453] Ovarian tumor antigen O644S (SEQ ID NO:238) was shown to be over-expressed in ovarian tumor tissue samples compared to normal tissues. Expression of O644S was similar in ovarian tumor samples compared to normal ovary. Mean expression ratios for O644S were as follows: ovarian tumor/normal ovary was 0.6 and ovarian tumor/other normal tissues was 5.8. These results indicate that O644S may be used in developing tumor immunotherapeutic and/or diagnostic agents.

[0454] Ovarian tumor antigen O645S (SEQ ID NO:238) was found to be over-expressed in over 70% of the ovarian tumors tested, and 100% of ovarian tumor SCID samples. No expression was detected in the normal tissues tested. This finding further supports the use of ovarian tumor antigen O645S in the diagnosis and treatment of ovarian cancer. Based on the excellent expression profile of this ovarian candidate, SEQ ID NO:238 was also run on an the Ovarian Metastatic Extended Panel, which included 14 primary ovarian tumors and 13 metastatic ovarian tumors. O645S was determined to be elevated in 10/14 (71%) of primary tumors and 11/13 (85%) metastatic tumors.

[0455] Ovarian tumor antigen O646S (SEQ ID NO:243) was found to be over-expressed in 100% of the ovarian tumors tested, 1/1 ovarian tumor cell lines (SKOV3-HTB77) and 100% of ovarian tumor SCID samples. Low-level expression was observed in 2/2 normal ovary samples tested, but no expression was detected in any other normal tissues tested. This finding further supports the use of ovarian tumor antigen O646S in the diagnosis and treatment of ovarian cancer, especially metastatic ovarian cancer. Based on the excellent expression profile of this ovarian candidate, SEQ ID NO:243 was also run on an the Ovarian Metastatic Extended Panel, which included 14 primary ovarian tumors and 13 metastatic ovarian tumors. O646S was determined to be elevated in 14/14 (100%) of primary tumors and 13/13 (100%) metastatic tumors.

[0456] Ovarian tumor antigen O647S (SEQ ID NO:234 and 235) was found to be over-expressed in over 80% of the ovarian tumors tested, and 100% of ovarian tumor SCID samples. O647S was also found to have low level expression in normal ovary, bronchus, brain/cerebellum, and heart. No expression was detected in any other normal tissues tested. This finding further supports the use of ovarian tumor antigen O647S in the diagnosis and treatment of ovarian cancer.

[0457] Ovarian tumor antigen O648S (SEQ ID NO:239) was found to be over-expressed in over 50% of the ovarian tumors tested. O648S was not expressed in normal ovary. Very low-level expression was seen in normal liver and pancreas. This finding further supports the use of ovarian tumor antigen O648S in the diagnosis and treatment of ovarian cancer.

[0458] Ovarian tumor antigen O651 S (SEQ ID NO:232) was found to be over-expressed in over 60% of the ovarian tumors tested, 1/1 ovarian tumor cell lines (SKOV3-HTB77) and 100% of ovarian tumor SCID samples. No expression was detected in the normal tissues tested. This finding further supports the use of ovarian tumor antigen O651S in the diagnosis and treatment of ovarian cancer.

[0459] Ovarian tumor antigen O645S (SEQ ID NO:238) was found to be over-expressed in over 70% of the ovarian tumors tested, and 100% of ovarian tumor SCID samples. No expression was detected in the normal tissues tested. This finding further supports the use of ovarian tumor antigen O645S in the diagnosis and treatment of ovarian cancer.

Example 19 LifeSeq Analysis of Ovarian Tumor Antigen 0590S

[0460] In Example 1 (Table VII) the DNA insert of clone 57886 was identified, and disclosed in SEQ ID NO:198 (606 bps in length), also referred to as O590S. Characterization of SEQ ID NO:198 by microarray analysis (Examples 2 and 9) indicated that corresponding mRNA was overexpressed in ovarian tumor tissue relative to normal tissues. Additional characterization by Northern blot analysis detected an mRNA transcript approximately 9.0 kb in size (Example 9). In this example, the DNA sequence for the ovarian tumor antigen O590S (SEQ ID NO:198) disclosed in Example 1 was used as a query to perform a BlastN search of the Incyte Genomics LifeSeq Gold database (LGtemplatesJan2001). This analysis identified an identical sequence match on template number 93744.1, corresponding to a 1740 base pair sequence, as is disclosed in SEQ ID NO:285. The gene bin, 93744, from which this match was identified contained 21 clones from various tumor libraries. Further analysis of the template 93744.1 sequence (SEQ ID NO:285), identified a −2 open reading frame that would translate a polypeptide with a predicted amino acid sequence disclosed in SEQ ID NO:286. In addition, this analysis confirmed that the open reading frame identified by SEQ ID NO:286 overlaps with and is contained within the nucleotide sequence of SEQ ID NO:198 corresponding to the ovarian tumor antigen 0590S.

Example 20 Analysis of Ovarian Tumor Antigen O664S

[0461] O644S (initially described in example 10 as SEQ ID NO:240, with extended open reading frames disclosed in SEQ ID NOS:280-282) was previously identified as having a good expression profile by microarray (see Example 18 for details) and was further analyzed by real-time PCR.

[0462] The first strand cDNA used in the quantitative real-time PCR was synthesized from 20 μg of total RNA that was treated with DNase I (Amplification Grade, Gibco BRLLife Technology, Gaithersburg, Md., using Superscript Reverse Transcriptase (RT) (Gibco BRL). Real-time PCR was performed with an ABIPRISM 7900 sequence detection system (PE Biosystems, Foster City, Calif.). The 7900 system uses SYBR™ green, a fluorescent dye that only intercalates into double stranded DNA, and a set of O644S specific forward and reverse primers. The increase in fluorescence was monitored during the whole amplification process. The optimal concentration of primers was determined using a checkerboard approach, and a pool of cDNAs from tumors was used in this process. The PCR was performed in 12.5 μl volumes that included 2.5 μl of SYBR green buffer, 2 μl of cDNA template and 2.5 μl each of the forward and reverse primer. The cDNAs used for the RT reactions were diluted 1:10 for O644S and 1:100 for the β-actin control. The expression of O644S in each of the tissue samples was represented by the comparative C_(T) (threshold cycle) method. C_(T) indicates the fractional cycle number at which the amount of amplified target reaches a fixed threshold. The C_(T) value of normal skin was used as a comparative reference in order to evaluate the over-expression levels seen with O644S.

[0463] O644S did not show over-expression in ovarian tumor tissue compared to normal tissue, however it did show higher expression in ovarian tumor tissue than in other normal tissue. As O644S is over-expressed in ovarian tumor tissue compared to normal tissues, it is a useful ovarian tumor antigen for the development of immunotherapeutic and/or diagnostic reagents. The high expression of O644S in both ovary tumor and normal ovary demonstrates that it would be a useful marker in the detection of metastatic cancer.

Example 21 O591S is Over-Expressed in Ovarian Cancer

[0464] This example describes how the ovarian antigen O591S, and antibodies specific for O591S, represent important therapeutic and diagnostic reagents useful in the detection of various types of carcinomas. The identification and characterization of O591S (SEQ ID NO: 214, encoding the protein of SEQ ID NO: 215) was described above (Example 1 and 4). In order to further characterize O591S, antibodies were generated against amino acid 14-141 of SEQ ID NI:215.

[0465] To generate these antibodies, amino acids 14-141 of SEQ ID NO:215 were expressed in an E. coli recombinant expression system and the cultures grown over-night in LB Broth, supplemented with the appropriate antibiotics, at 37° C. in a shaking incubator. Following the incubation, 10 mls of the over-night culture was added to 500 ml of 2× YT, supplemented with the appropriate antibiotics, in a two-liter baffled Erlenmeyer flask. When the optical density (at 560 nm) of the cultures reached 0.4-0.6, the cells were induced with IPTG (1 mM). Fours hours post-induction with IPTG, the cells were harvested by centrifugation, followed by washing with phosphate buffered saline (PBS). The supernatant was then discarded and the cells either frozen for future use, or immediately processed.

[0466] To process the cells, 20 μl of lysis buffer was added to the cell pellet and the mixture vortexed. To break open the E. coli cells, the mixture was run through a French Press at a pressure of 16,000 psi. The mixture was then centrifuged again and the supernatant and cell pellet checked by SDS-PAGE for the partitioning of the O591S-specific recombinant protein.

[0467] To isolate the O591S proteins localized to the cell pellet, the pellet was resuspended in 10 mM Tris pH 8.0, 1% CHAPS and the inclusion body pellet was washed and centrifuged. This procedure was repeated twice more. The washed inclusion body pellet was solubilized with either 8 M urea or 6 M guanidine HCl containing 10 mM Tris, pH 8.0 plus 10 mM imidazole. The solubilized protein was added to 5 ml of nickel-chelate resin (Qiagen) and incubated for 45 minutes to 1 hour at room temperature with continuous agitation. After incubation, the resin and protein mixture were poured through a disposable column and the flow through collected. The column was then washed with 10-20 column volumes of the solubilized buffer. The antigen was then eluted from the column using 8 M urea, 10 mM Tris, pH 8.0, and 300 mM imidazole and collected in 3 ml fractions.

[0468] A SDS-PAGE gel was run to determine which fractions to pool for further purification. As a final purification step, a strong anion resin, such as Hi-Prep Q (Biorad) was equilibrated with the appropriate buffer and the pooled fractions from above were loaded onto the column. Each antigen was eluted off the column with an increasing salt gradient. Fractions were collected as the column was run and second SDS-PAGE gel was run to determine which fractions from the column to pool. The pooled fractions were dialyzed against 10 mM Tris, pH 8.0.

[0469] In order to generate polyclonal anti-sera against O591 S, 400 μg of O591S protein was combined with 100 μg of muramydipeptide (MDP). An equal volume of Incomplete Freund's Adjuvant (IFA) was added and the resulting solution mixed. Every four weeks, animals were boosted with 100 μg of antigen mixed with an equal volume of IFA. Seven days following each boost, the animal was bleed, and the sera isolated by incubating the blood at 4° C. for 12-24 hours followed by centrifugation.

[0470] In order to characterize the rabbit polyclonal anti-sera, 96 well plates were coated with antigen by incubating with 50 μl (typically 1 μg) at 4° C. for 20 hours. Following the incubation, 250 μl of BSA blocking buffer was added to the wells and incubated at room temperature for 2 hours. The plates were then washed 6 times with PBS/0.01% Tween.

[0471] Fifty microliters of the diluted sera was added to each well and incubated at room temperature for 30 minutes. Plates were washed as described above, before 50 μl of goat-anti-rabbit horse radish peroxidase (HRP) at a 1:10,000 dilution was added and incubated for 30 minutes. Plates were washed as described above and 100 μl of TMB microwell Peroxidase Substrate was added to each well. Following a 15-minute incubation in the dark at room temperature, the colorimatric reaction was stopped with 100 μl of H₂SO₄ and immediately read at 450 nm. All polyclonal antibodies tested demonstrated specific immunoreactivity to the appropriate antigen.

[0472] Immunohistochemical analysis (IHC) of O591 S expression was then performed to determine the tissue specificity of O591 S. For IHC, paraffin-embedded formalin fixed tissues were slice into 8-micron sections. Steam heat induced epitope retrieval (SHIER) in 0.1 M sodium citrate buffer (ph 6.0) was used for optimal staining conditions. Sections were incubated with 10% serum/PBS for 5 minutes. Primary antibody was added to each section for 25 minutes at a range of concentrations, followed by a 25-minute incubation with an anti-rabbit biotinylated antibody. Endogenous peroxidase activity was blocked by three 1.5-minute incubations with hydrogen peroxidase. The avidin biotin complex/horse radish peroxidase (ABC/HRP) system was used along with DAB chromogen to visualize antigen expression. The slides were then counterstained with hematoxylin.

[0473] Of the tissues tested, 4/5 primary ovarian cancers and 3/5 metastatic ovarian samples tested positive for O591S immunoreactivity. Of the normal tissue samples tested, 2/5 normal ovary samples were positive, and 1/1 normal bronchial epithelium was positive. Normal alveolar epithelium, kidney, colon, liver, and heart were all negative for O591S immunoreactivity.

[0474] These findings further validate the use of O591S in any of a variety of illustrative diagnostic and therapeutic embodiments described herein.

Example 22 Cell Surface Expression of the Ovarian Tumor Antigen, O591S

[0475] The identification and characterization of O591S (SEQ ID NO: 214, encoding the protein of SEQ ID NO: 215) was described above (Example 1 and 4). To characterize the cell surface expression of O591S, cell lines were either transfected with full-length O591 S cDNA or infected with an adenoviral expression construct expressing O591S cDNAs. These cell lines were then stained using purified rabbit polyclonal anti-O591S antibodies raised against synthetic O591S peptides, and surface expression analyzed by FACS. The O591S polyclonal antibodies were raised against the following peptides; peptide 1 (SEQ ID NO:291) corresponding to amino acid positions 26-55 of the O591S protein sequence (SEQ ID NO:215), peptide 2 (SEQ ID NO:292) corresponding to amino acid positions 53-78 of the O591S protein sequence (SEQ ID NO:215), and peptide 3 (SEQ ID NO:293) corresponding to amino acid positions 103-129 of O591S protein sequence (SEQ ID NO:215). Polyclonal antibodies were generated essentially as described in Examples 17 and 21 of the present application.

[0476] Cell surface expression of O591S was determined as follows:

[0477] 1. oNXA cells were transfected by CaPO₄ precipitation with (a) a negative control cDNA cloned into the expression vector pBIB, or (b) O591S cDNA cloned into the expression vector pBIB. Seventy-two hours post-transfection, the cells were harvested and stained with either (i) control rabbit polyclonal antibody, (ii) rabbit polyclonal anti-O591S antibody, or (iii) secondary antibody (anti-rabbit-FITC) alone. All cells transfected with an expression vector containing O591S stained using the O591S specific polyclonal antibodies, demonstrating surface expression of O591S.

[0478] 2. oNXA cells were transfected by CaPO₄ precipitation with either; pBIB/O591S (O591S cDNA cloned into the expression vectors pBIB), pcDNA/O591S (O591S cDNA cloned into the expression vector, pcDNA3), or pCEP/O591S (O591S cDNA cloned into the expression vector pCEP4). Seventy-two hours post-transfection, cells were harvested and stained with either (i) control rabbit polyclonal antibody or (ii) rabbit polyclonal anti-O591S antibody. O591S was detected on the surface of all cells transfected with O591S specific sequences. O591S expression levels were shown to be highest with the episomal replicating vector pcDNA4.

[0479] 3. oNXA and 293 cells were transfected by CaPO₄ precipitation with pcDNA/O591S (O591S cDNA cloned into the expression vector pc DNA3). Seventy-two hours post-transfection, the cells were harvested and stained with either (i) control rabbit polyclonal antibodies, or (ii) rabbit polyclonal anti-O519S antibody. The cells were than analyzed using FACS analysis. Both oNXA and 293 cells transfected with O591S demonstrated cell surface expression of O591S.

[0480] 4. VA13 cells and oNXA cells were infected (MOI of 10:1) with O591S/adenovirus (O591S cDNA cloned into the adenoviral expression vector). Seventy-two hours post-infection, the cells were harvested and stained with either, (i) control rabbit polyclonal antibody, or (ii) rabbit polyclonal anti-O591S antibody. The cells were then analyzed using FACS. Cells infected with O591S/adenovirus demonstrated cell surface staining specific for O591S.

[0481] To further characterize that O591S was a surface expressed protein, oNXA cells were transfected by CaPO₄ precipitation with pBIB/O591S (O591S cDNA cloned into the expression vector pBIB). Seventy-two hours post-transfection the cells were harvested and incubated for an additional one hour in either the presence or absence of phoshatidylinositol phospholipae C (PI-PLC), an enzyme known to cleave glycosyl-phosphatidylinositol (GPI)-linked proteins. GPI-linked proteins are known to be surface expressed proteins. Following incubation with PI-PLC, the cells were washed and either stained with (i) rabbit polyclonal anti-O591S antibody, or (ii) secondary antibody (anti-rabbit-FITC) alone, and analyzed by FACS for O591S cell surface expression. Analysis demonstrated that cells treated with PI-PLC were negative for the cell surface expression of O591S. further demonstrating that this protein is a surface expressed protein. Analysis of the O591S protein sequence (SEQ ID NO:215) revealed that the enzyme PI-PLC cleaved at either the Arg at position 114 of SEQ ID NO:215, resulting in the generation of a liberated 114 amino acid fragment, the sequence of which is disclosed in SEQ ID NO:289, and theoretically a 27 amino acid cell associated fragment (residues 115-141 of SEQ ID NO:215) or at the Gly at position 115 of SEQ ID NO:215, resulting in the generation of a 115 amino acid fragment, the sequence of which is disclosed in SEQ ID NO:290 and theoretically a 26 amino acid cell associated fragment (residues 116-141 of SEQ ID NO:215).

[0482] These data demonstrate that O591S is a surface expressed, GPI-linked protein, making the sequence a target for therapeutic antibodies.

[0483] From the foregoing it will be appreciated that, although specific embodiments of the invention have been described herein for purposes of illustration, various modifications may be made without deviating from the spirit and scope of the invention. Accordingly, the invention is not limited except as by the appended claims.

0 SEQUENCE LISTING <160> NUMBER OF SEQ ID NOS: 293 <210> SEQ ID NO 1 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 303, 370, 377, 382 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 1 caacctcact agtaaatgaa agaaatattg taatttgtat ttgatctgct gggtctttgg 60 agtcagaact ggttttatca gcagtttgat cttctgaggt ctggtatgta gtttgctggc 120 ccacagaacc ttcacgtgta ttcacagcct caatgccata aggaaactct tttagaagtt 180 ctgacagctg gtcatgtagg tataagacag gtgccttatc actgtggatt tcatttcttg 240 caggatcttg gggagtatag ttgctggatg catctatttc ctgagggtaa atatcctcct 300 ggncgacgcg gccgctcgag tctagagggc ccgtttaaac ccgctgatca gcctcgactg 360 tgccttctan ttgccancca tntgttgttt gcccct 396 <210> SEQ ID NO 2 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 2 cgaccaaaaa gtaaactcca agtgaacatc aaatcaaatc taatcctttt ggccacatga 60 ctggttgttc tttatctcat agttacaatg aatcatataa actgtagact gccactacca 120 cgatacttct gtgacacaga aggaatgtcc tatttgccta tctatctgag gaatgttaaa 180 tagagaaaaa tagattataa aacaacctgg aggtcacagg attctgagat aatccctctg 240 ttaaaaaaca tctgaacagc aaatgtccaa tctgtaataa aatagttaaa ggtccaagtc 300 aagtccactt ctacttggct ggcccagcac aagaaatcta acagcacttt gtaatcattt 360 tgcttttcta attttcccgg aggacatggg ccattg 396 <210> SEQ ID NO 3 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 22, 28, 29, 30, 33, 36, 41, 43, 45, 46, 53, 56, 58, 61, 64, 69, 70, 74, 75, 78, 83, 84, 85, 102, 143, 335 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 3 cgcccttttt tttttttttt tnattggnnn aantcncttt nantnnaaaa acntgnangg 60 naancccann cccnnggnac cannnccagg agttgggtgg anactgagtg gggtttgtgt 120 gggtgagggg gcatctactc ctnttgcaac aagccaaaag tagaacagcc taaggaaaag 180 tgacctgcct tggagcctta gtccctccct tagggccccc tcagcctacc ctatccaagt 240 ctgaggctat ggaagtctcc ctcctagttc actagcaggt tccccatctt ttccaggctg 300 cccctagcac tccacgtttt tctgaaaaaa tctanacagg ccctttttgg gtacctaaaa 360 cccagctgag gttgtgagct tgtaaggtaa agcaag 396 <210> SEQ ID NO 4 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 13, 15, 21, 27, 34, 37, 41, 57, 58, 59, 63, 64, 71, 72, 77, 78, 83, 87, 93, 170, 207, 210, 308, 379, 382, 389, 391, 392, 393, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 4 gaccaatcct tgncncacta ncaaaangac cccnctnacc nccaggaact gaacctnnnt 60 gtnnacctcc nnctgcnnag ccntatntcc aanatcaccc accgtatcca ctgggaatct 120 gccagcctcc tgcgatcaga agagaccaat cgaaaatgag ggtttcacan tcacagctga 180 aggaaaaggc caaggcacct tgtcggnggn gacaatgtac catgctaagg ccaaagatca 240 actcacctgt aataaattcg acctcaaggt caccataaaa ccagcaccgg aacagaaaaa 300 gaggcctnag gatgcccaag aaacactttt gatcctttga aaactgtacc aaggtaccgg 360 ggggagaccc aggaaaggnc cnttatgtnt nnntnt 396 <210> SEQ ID NO 5 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 135, 172, 343, 348, 354, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 5 gacgccggag ctgccgcgcc agtcgcctag caggtcctct accggcttat tcctgtgccg 60 gatcttcatc ggcacagggg ccactgagac gtttctgcct ccctctttct tcctccgctc 120 tttctcttcc ctctngttta gtttgcctgg gagcttgaaa ggagaaagca cnggggtcgc 180 cccaaaccct ttctgcttct gcccatcaca agtgccacta ccgccatggg cctcactatc 240 tcctccctct tctcccgact atttggcaag aagcagatgc gcattttgat ggttggattg 300 gatgctgctg gcaagacaac cattcttgat aaactgaaag tanggganat aagnaccacc 360 atttctacca ttgggtttaa tgggggaaac agtana 396 <210> SEQ ID NO 6 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 212 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 6 acgggaggcg ccgggaagtc gacggcgccg gcggctcctg caggaggcca ctgtctgcag 60 ctcccgtgaa gatgtccact ccagacccac ccctgggcgg aactcctcgg ccaggtcctt 120 ccccgggccc tgcccttccc ctggagccat gctgggccct agcccgggtc cctcgccggg 180 ctccgcccac agcatgatgg ggcccagccc angggccgcc ctcagcagga caccccatcc 240 ccacccaggg gcctggaggg taccctcagg acaacatgca ccagatgcac aagcccatgg 300 agtccatgca tgagaagggc atgtcggacg acccgcgcta caaccagatg aaaggaatgg 360 ggatgcggtc agggggccat gctgggatgg ggcccc 396 <210> SEQ ID NO 7 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 7 acccgagagt cgtcggggtt tcctgcttca acagtgcttg gacggaaccc ggcgctcgtt 60 ccccaccccg gccggccgcc catagccagc cctccgtcac ctcttcaccg caccctcgga 120 ctgccccaag gcccccgccg ccgctccagc gccgcgcagc caccgccgcc gccgccgcct 180 ctccttagtc gccgccatga cgaccgcgtc cacctcgcag gtgcgccaga actaccacca 240 ggactcagag gccgccatca accgccagat caacctggag ctctacgcct cctacgttta 300 cctgtccatg tcttactact ttgaccgcga tgatgtggct ttgaagaact ttgccaaata 360 ctttcttcac caatctcatg aggagaggga acatgc 396 <210> SEQ ID NO 8 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 8 cgacaacaag gttaatacct tagttcttaa catttttttt ctttatgtgt agtgttttca 60 tgctaccttg gtaggaaact tatttacaaa ccatattaaa aggctaattt aaatataaat 120 aatataaagt gctctgaata aagcagaaat atattacagt tcattccaca gaaagcatcc 180 aaaccaccca aatgaccaag gcatatatag tatttggagg aatcaggggt ttggaaggag 240 tagggaggag aatgaaggaa aatgcaacca gcatgattat agtgtgttca tttagataaa 300 agtagaaggc acaggagagg tagcaaaggc caggcttttc tttggttttc ttcaaacata 360 ggtgaaaaaa acactgccat tcacaagtca aggaac 396 <210> SEQ ID NO 9 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 321, 344 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 9 tcgacatcgc ggcaactttt tgcggattgt tcttgcttcc aggctttgcg ctgcaaatcc 60 agtgctacca gtgtgaagaa ttccagctga acaacgactg ctcctccccc gagttcattg 120 tgaattgcac ggtgaacgtt caagacatgt gtcagaaaga agtgatggag caaagtgccg 180 ggatcatgta ccgcaagtcc tgtgcatcat cagcggcctg tctcatcgcc tctgccgggt 240 accagtcctt ctgctcccca gggaaactga actcagtttg catcagctgc tgcaacaccc 300 ctctttgtaa cgggccaagg nccaaaaaaa ggggaaagtt ctgncctcgg ccctcaggcc 360 agggctccgc accaccatcc tgttcctcaa attagc 396 <210> SEQ ID NO 10 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 115, 116, 117, 130, 138, 142, 143, 144, 145, 146, 153, 157, 158, 159, 160, 164, 175, 176, 177, 178, 179, 183, 187, 197, 198, 202, 203, 204, 205, 206, 211, 212, 213, 215, 216, 217, 220, 221, 222, 226, 231, 234, 236, 237, 245, 246, 247 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 250, 255, 264, 266, 267, 268, 269, 270, 271, 272, 279, 284, 297, 303, 304, 305, 308, 315, 317, 318, 319, 320, 321, 322, 323, 333, 334, 337, 338, 342, 343, 368, 372, 374, 380, 381, 391, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 10 cctttttttt tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt 60 tttttttttt tttttttttt tttttttttt tttttttttt ttttaaaaaa aaaannnttt 120 tttttttttn aaaaaaangg gnnnnntttt ttncccnnnn gggngggggg ggggnnnnnt 180 ttnaaanaaa aaaaccnnaa annnnngggg nnnannnaan nncccncccc naancnntaa 240 aaaannnggn aaaanagggg gggnannnnn nnggggggna aaantttttt ttttttnaag 300 ggnnnggnaa aaaantnnnn nnnttttttt ttnnaanngg gnnaaaaaaa aaaaaaaaaa 360 attttttngg gntnaggggn ngggggaaaa ncccna 396 <210> SEQ ID NO 11 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 11 agaacacagg tgtcgtgaaa actaccccta aaagccaaaa tgggaaagga aaagactcat 60 atcaacattg tcgtcattgg acacgtagat tcgggcaagt ccaccactac tggccatctg 120 atctataaat gcggtggcat cgacaaaaga accattgaaa aatttgagaa ggaggctgct 180 gagatgggaa agggctcctt caagtatgcc tgggtcttgg ataaactgaa agctgagcgt 240 gaacgtggta tcaccattga tatctccttg tggaaatttg agaccagcaa gtactatgtg 300 actatcattg atgccccagg acacagagac tttatcaaaa acatgattac agggacatct 360 caggctgact gtgctgtcct gattgttgct gctggt 396 <210> SEQ ID NO 12 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 12 cgaaaacctt taaaccccgg tcatccggac atcccaacgc atgctcctgg agctcacagc 60 cttctgtggt gtcatttctg aaacaagggc gtggatccct caaccaagaa gaatgtttat 120 gtcttcaagt gacctgtact gcttggggac tattggagaa aataaggtgg agtcctactt 180 gtttaaaaaa tatgtatcta agaatgttct agggcactct gggaacctat aaaggcaggt 240 atttcgggcc ctcctcttca ggaatcttcc tgaagacatg gcccagtcga aggcccagga 300 tggcttttgc tgcggccccg tggggtagga gggacagaga gacagggaga gtcagcctcc 360 acattcagag gcatcacaag taatggcaca attctt 396 <210> SEQ ID NO 13 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 13 accacaggct ggccacaaga agcgctggag tgtgctggcg gctgcaggcc tacggggcct 60 ggtccggctg ctgcacgtgc gtgccggctt ctgctgcggg gtcatccgag cccacaagaa 120 ggccatcgcc accctgtgct tcagccccgc ccacgagacc catctcttca cggcctccta 180 tgacaagcgg atcatcctct gggacatcgg ggtgcccaac caggactacg aattccaggc 240 cagccagctg ctcacactgg acaccacctc tatccccctg cgcctctgcc ctgtcgcctc 300 ctgcccggac gcccgcctgc tggccggctg cgagggcggc tgctgctgct gggacgtgcg 360 gctggaccag ccccaaaaga ggagggtgtg tgaagt 396 <210> SEQ ID NO 14 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 14 acggcgtcct cgtggaagtg acatcgtctt taaaccctgc gtggcaatcc ctgacgcacc 60 gccgtgatgc ccagggaaga cagggcgacc tggaagtcca actacttcct taagatcatc 120 caactattgg atgattatcc gaaatgtttc attgtgggag cagacaatgt gggctccaag 180 cagatgcagc agatccgcat gtcccttcgc gggaaggctg tggtgctgat gggcaagaac 240 accatgatgc gcaaggccat ccgagggcac ctggaaaaca acccagctct ggagaaactg 300 ctgcctcata tccgggggaa tgtgggcttt gtgttcacca aggaggacct cactgagatc 360 agggacatgt tgctggccaa taaggtgcca gctgct 396 <210> SEQ ID NO 15 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 333 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 15 accgcgcggg cacagggtgc cgctgaccga ggcgtgcaaa gactccagaa ttggaggcat 60 gatgaagact ctgctgctgt ttgtggggct gctgctgacc tgggagagtg ggcaggtcct 120 gggggaccag acggtctcag acaatgagct ccaggaaatg tccaatcagg gaagtaagta 180 cgtcaataag gaaattcaaa atgcttgtca acggggtgaa acagataaag actctcatag 240 aaaaaacaaa cgaagagcgc aagacactgc tcagcaacct agaagaagcc aagaagaaga 300 aagaggatgc cctaaatgag accagggaat canagacaaa gctgaaggag ctcccaggag 360 tgtgcaatga gaccatgatg gccctctggg aagagt 396 <210> SEQ ID NO 16 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 114, 121, 122, 123, 127, 134, 136, 138, 140, 141, 142, 143, 144, 148, 163, 166, 172, 173, 174, 176, 177, 183, 184, 185, 187, 195, 196, 198, 199, 202, 203, 206, 213, 214, 215, 216, 217, 218, 219, 223, 225, 226, 227, 229, 230, 236, 238 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 239, 252, 256, 257, 261, 262, 268, 269, 273, 278, 280, 288, 289, 290, 292, 293, 303, 312, 325, 327, 333, 335, 336, 341, 342, 347, 354, 359, 365, 371, 383, 384, 386, 388, 391 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 16 tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt 60 tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt tttngggggg 120 nnnaaanttt tttntnanan nnnngggnaa aaaaaaaaaa aanaangggg gnnntnnggc 180 ccnnnanaaa aaaanngnna annaancccc ccnnnnnnnc ccncnnntnn ggaaananna 240 aaaccccccc cngggnnggg nnaaaaannc ccnggggnan tttttatnnn annccccccc 300 ccnggggggg gnggaaaaaa aaaantnccc ccnannaaaa nnggggnccc cccnttttnc 360 aaaanggggg nccgggcccc ccnnantntt nggggg 396 <210> SEQ ID NO 17 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 17 accacactaa ccatatacca atgatggcgc gatgtaacac gagaaagcac ataccaaggc 60 caccacacac cacctgtcca aaaaggcctt cgatacggga taatcctatt tattacctca 120 gaagtttttt tcttcgcagg atttttctga gccttttacc actccagcct agcccctacc 180 ccccaactag gagggcactg gcccccaaca ggcatcaccc cgctaaatcc cctagaagtc 240 ccactcctaa acacatccgt attactcgca tcaggagtat caatcacctg agctcaccat 300 agtctaatag aaaacaaccg aaaccaaata attcaagcac tgcttattac aattttactg 360 ggtctctatt ttaccctcct acaagcctca gagtac 396 <210> SEQ ID NO 18 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 51, 54, 66, 81, 86, 98, 106, 111, 117, 124, 129, 133, 135, 150, 151, 154, 159, 161, 172, 179, 181, 183, 185, 220, 223, 229, 238, 258, 259, 264, 282, 289, 292, 294, 299, 303, 311, 315, 329, 343, 349, 351, 353, 361, 369, 370, 389, 392 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 18 tttttttttt tttttttttt tttttttttt tttttttttt ttttttttta ntcnaaaggg 60 gaaggnccct ttttattaaa nttggncatt ttactttnct tttttnaaaa ngctaanaaa 120 aaanttttnt ttntncttaa aaaaaccctn natntcacna ncaaaaaaaa cnattcccnc 180 ntncnttttg tgataaaaaa aaaggcaatg gaattcaacn tancctaana aaactttncc 240 tgggaggaaa aaaaattnnt ccgngggaaa cacttggggc tntccaaant gnanccatnc 300 tangaggacc ntctntaaga tttccaaang aaaccccttc ctnccaaang nantaccccg 360 ntgcctacnn cccataaaaa aaacctcanc cntaan 396 <210> SEQ ID NO 19 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 47, 69, 75, 80, 83, 87, 88, 90, 92, 102, 104, 108, 116, 121, 130, 138, 139, 142, 153, 156, 158, 162, 165, 166, 180, 192, 193, 195, 201, 224, 226, 232, 235, 237, 241, 248, 251, 253, 256, 269, 272, 274, 277, 284, 287, 290, 292, 297 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 299, 305, 306, 315, 323, 324, 326, 332, 351, 368, 377, 380, 383, 387, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 19 tttttttttt tttttttttt tttttttttt tttttttttt ttttttntgg tctgggcttt 60 tattttacna aaaanctaan ggnaaanntn cnttaaacta antngaanac aaagtnttaa 120 ngaaaaaggn ctgggggnnt cntttacaaa aanggncngg gncanntttg ggcttaaaan 180 ttcaaaaagg gnncntcaaa ngggtttgca tttgcatgtt tcancnctaa ancgnangaa 240 naaacccngg ngnccnctgg gaaaagttnt tnanctncca aaanatnaan tntttgnanc 300 agggnntttt tgggnaaaaa aannanttcc anaaactttc catcccctgg ntttgggttc 360 ggccttgngt tttcggnatn atntccntta angggg 396 <210> SEQ ID NO 20 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 29, 43, 49, 53, 55, 75, 81, 100, 110, 111, 125, 129, 160, 162, 168, 246, 277 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 20 tttttttttt tttttttttt ttttttctna acaaaccctg ttnttgggng ggngngggta 60 taatactaag ttganatgat ntcatttacg ggggaaggcn ctttgtgaan naggccttat 120 ttctnttgnc ctttcgtaca gggaggaatt tgaagtaaan anaaaccnac ctggattact 180 ccggtctgaa ctcaaatcac gtaggacttt aatcgttgaa caaacaaacc tttaatagcg 240 gctgcnccat tgggatgtcc tgatccaaca tcgaggncgt aaaccctatt gttgatatgg 300 actctaaaaa taggattgcg ctgttatccc tagggtaact tgttcccgtg gtcaaagtta 360 ttggatcaat tgagtataag tagttcgctt tgactg 396 <210> SEQ ID NO 21 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 6, 9, 18, 23, 37, 43, 48, 55, 65, 73, 75, 103, 110, 117, 123, 125, 134, 153, 182, 195, 202, 205, 213, 216, 223, 239, 249, 276, 293, 294, 302, 307, 344, 356, 359, 369, 374, 381, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 21 acatanatnt tatactanca ttnaccatct cacttgnagg aanactanta tatcnctcac 60 acctnatatc ctncntacta tgcctagaag gaataatact atngctgttn attatancta 120 ctntnataac cctnaacacc cactccctct tanccaatat tgtgcctatt gccatactag 180 tntttgccgc ctgcnaagca gnggngggcc tanccntact agnctcaatc tccaacacnt 240 atggcctana ctacgtacat aacctaaacc tactcnaatg ctaaaactaa tcnncccaac 300 anttatntta ctaccactga catgactttc caaaaaacac atantttgaa tcaacncanc 360 cacccacanc ctanttatta ncatcatccc cntact 396 <210> SEQ ID NO 22 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 17, 244 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 22 tttttttttt ttttganaaa agccggcata aagcactttt attgcaataa taaaacttga 60 gactcataaa tggtgctggg ggaagggtgc agcaacgatt tctcaccaaa tcactacaca 120 ggacagcaaa ggggtgagaa ggggctgagg gaggaaaagc caggaaactg agatcagcag 180 agggagccaa gcatcaaaaa acaggagatg ctgaagctgc gatgaccagc atcattttct 240 taanagaaca ttcaaggatt tgtcatgatg gctgggcttt cactgggtgt taagtctaca 300 aacagcacct tcaattgaaa ctgtcaatta aagttcttaa gatttaggaa gtggtggagc 360 ttggaaagtt atgagattac aaaattcctg aaagtc 396 <210> SEQ ID NO 23 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 23 acaaaggcgg ttccaagcta aggaattcca tcagtgcttt tttcgcagcc accaaattta 60 gcaggcctgt gaggttttca tatcctgaag agatgtattt taaagctttt tttttttaat 120 gaaaaaatgt cagacacaca caaaagtaga atagtaccat ggagtcccca cgtacccagc 180 ctgcagcttc aacagttacc acatttgcca accggagaga ctgccaaggc aggaaaaagc 240 cctggaaagc ccacggcccc tttttccctt gggtcagagg ccttagagct ggctgccaaa 300 gcagccaacc aaaggggcag ctcagctcct tcgtggcacc agcagtgttc ctgatgcagt 360 tgaagagttg atgtctttga caacatacgg acactg 396 <210> SEQ ID NO 24 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 313, 337, 340, 350, 351, 352, 353, 354, 355, 356, 366, 376, 377, 378, 382, 384, 385, 387, 389, 390, 392, 393, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 24 cgactatcct ctcagattct tatctggcac taatttataa ctattatatt atcagagact 60 atgtagcaat atatcagtgc acaggcgcat cccaggcctg tacagatgta tgtctacacg 120 taagtataaa tgaatttgca taccaggttt tacacttgca tctctaatag agattaaaaa 180 caacaaattg gcctcttcct aagtatatta atatcattta tccttacatt ttatgcctcc 240 ccctaaatta atgactgagt tggtggaaag cggctaggtt ttattcatac tgttttttgt 300 tctcaacttc aanagtaatc tacctctgaa aaatttntan tttaatattn nnnnnnagga 360 atttgngcca ctttannnct tncnntntnn tnnccn 396 <210> SEQ ID NO 25 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 90, 125, 136, 278, 299, 301, 305, 344, 347, 353, 355, 356, 357, 359, 360, 361, 365, 369, 378, 380, 381, 382, 383, 384, 385, 386, 391, 392, 393, 395, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 25 tttttttttt tttttttttt gtcttttaaa aaatataaaa gtgttattat tttaaaacat 60 caagcattac agactgtaaa atcaattaan aactttctgt atatgaggac aaaaatacat 120 ttaanacata tacaanaaga tgctttttcc tgagtagaat gcaaactttt atattaagct 180 tctttgaatt ttcaaaatgt aaaataccaa ggctttttca catcagacaa aaatcaggaa 240 tgttcacctt cacatccaaa aagaaaaaaa aaaaaaancc aattttcaag ttgaagttna 300 ncaanaatga tgtaaaatct gaaaaaagtg gccaaaattt taanttncaa canannngnn 360 ncagntttna tggatctntn nnnnnncttc nnntnn 396 <210> SEQ ID NO 26 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 313, 314, 316, 318, 321, 343, 344, 352, 353, 356, 363, 366, 370, 372, 373, 374, 375, 377, 378, 379, 383, 384, 385, 386, 387, 391, 393, 394, 395, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 26 gacgctcccc cctccccccg agcgccgctc cggctgcacc gcgctcgctc cgagtttcag 60 gctcgtgcta agctagcgcc gtcgtcgtct cccttcagtc gccatcatga ttatctaccg 120 ggacctcatc agccacgatg agatgttctc cgacatctac aagatccggg agatcgcgga 180 cgggttgtgc ctggaggtgg aggggaagat ggtcagtagg acagaaggta acattgatga 240 ctcgctcatt ggtggaaatg cctccgctga aggccccgag ggcgaaggta cccgaaagca 300 cagtaatcac tgnngncnat nttgtcatga accatcacct gcnngaaaca annttnacaa 360 aanaancctn cnnnnannnc ctnnnnnatt ncnnnn 396 <210> SEQ ID NO 27 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 49, 61, 66, 73, 75, 99, 102, 103, 105, 107, 120, 124, 126, 129, 138, 139, 141, 147, 155, 157, 162, 165, 175, 187, 191, 193, 198, 207, 217, 218, 220, 221, 223, 226, 231, 232, 245, 257, 259, 260, 263, 266, 271, 287, 305, 306, 307, 308 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 321, 330, 332, 335, 342, 343, 344, 345, 349, 350, 351, 352, 354, 355, 356, 357, 365, 366, 367, 370, 371, 372, 373, 374, 375, 376, 377, 378, 379, 380, 381, 382, 383, 386, 387, 388, 389, 391, 392, 393, 394, 395, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 27 tttttttttt tttttttttt tttttttttt tttttttttt tggctaaant ttatgtatac 60 nggttnttca aangnggggg aggggggggg gcatccatnt anncncncca ggtttatggn 120 gggntnttnt actattanna nttttcnctt caaancnaag gnttntcaaa tcatnaaaat 180 tattaanatt ncngctgnta aaaaaangaa tgaaccnncn nanganagga nntttcatgg 240 ggggnatgca tcggggnann ccnaanaacc ncggggccat tcccganagg cccaaaaaat 300 gtttnnnnaa aaagggtaaa nttacccccn tnaantttat annnnaaann nnannnnagc 360 ccaannnttn nnnnnnnnnn nnnccnnnna nnnnnn 396 <210> SEQ ID NO 28 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 278, 283, 298, 309, 326, 331, 338, 351, 355, 356, 357, 358, 360, 371, 377, 378, 383, 386, 387, 391, 393, 394, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 28 cgaccttttt tttttttttt atagatgaaa gagggtttat ttattaatat atgatagcct 60 tggctcaaaa aagacaaatg agggctcaaa aaggaattac agtaacttta aaaaatatat 120 taaacatatc caagatccta aatatattat tctccccaaa agctagctgc ttccaaactt 180 gatttgatat tttgcatgtt ttccctacgt tgcttggtaa atatatttgc ttctcctttc 240 tgcaatcgac gtctgacagc tgatttttgc tgttttgnca acntgacgtt tcaccttntg 300 tttcaccant tctggaggaa ttgttnaaca ncttacanca ctgccttgaa naaannnnan 360 gcctcaaaag ntcttgnnct atnctnnttc ntnnnt 396 <210> SEQ ID NO 29 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 329, 334, 361, 386, 390 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 29 gacttgctca tttagagttt gcaggaggct ccatactagg ttcagtctga aagaaatctc 60 ctaatggtgc tatagagagg gaggtaacag aaagactctt ttagggcatt tttctgactc 120 atgaaaagag cacagaaaag gatgtttggc aatttgtctt ttaagtctta accttgctaa 180 tgtgaatact gggaaagtga tttttttctc actcgttttt gttgctccat tgtaaagggc 240 ggaggtcagt cttagtggcc ttgagagttg cttttggcat ttaaatattc taagagaatt 300 aactgtattt cctgtcacct attcactant gcangaaata tacttgctcc aaataagtca 360 ntatgagaag tcactgtcaa tgaaanttgn tttgtt 396 <210> SEQ ID NO 30 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 28, 83, 126, 138, 254, 275, 298, 310, 311, 353, 363, 374, 379, 393 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 30 tttttttttt tttttttttg aaatttanaa acaaatttta tttaagatct gaaatacaat 60 tcctaaaata tcaacttttc canaaaaccg tggctacaca ataatgcatt gcctctatca 120 tgttanaacg tgcattanac tcaaatacaa aaaccatgaa acaaatcacc atccttcaac 180 aatttgagca aagatagaat gcctaagaac aacatagatg gacttgcaga ggatgggctg 240 ttttacttca agcnccataa aaaaaaaaaa gagcncaaat gcattgggtt ttcaggtnta 300 tacattaagn ngaacctttg gcactaggaa tcagggcgtt ttgtcacata gcnttaacac 360 atnttaaaaa attntgtant gtcaaaggga tangaa 396 <210> SEQ ID NO 31 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 285, 287, 350, 362, 365, 377, 378, 382, 388, 390, 393 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 31 gacgggccag ggccatctgg aaagggaact cggcttttcc agaacgtggt ggatcatctg 60 tcgggtgtgt ggtgaacacg ttcagttcat cagggcctac gctccgggaa ggggccccca 120 gctgtggctc tgccatgccg ggctgtgttt gcagctgtcc gagtctccat ccgcctttag 180 aaaaccagcc acttcttttc ataagcactg acagggccca gcccacagcc acaggtgcga 240 tcagtgcctc acgcaggcaa atgcactgaa acccaggggc acacncncgc agagtgaaca 300 gtgagttccc ccgacagccc acgacagcca ggactgccct ccccaccccn ccccgacccc 360 angancacgg cacacanntc ancctctnan ctngct 396 <210> SEQ ID NO 32 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 341 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 32 cgactggcct cataccttgt ctacacagtc cctgcacagg gttcctaacc tgtggttagt 60 aaagaatgtc actttctaac aggtctggaa gctccgagtt tatcttggga actcaagagg 120 agaggatcac ccagttcaca ggtatttgag gatacaaacc cattgctggg ctcggcttta 180 aaagtcttat ctgaaattcc ttgtgaaaca gagtttcatc aaagccaatc caaaaggcct 240 atgtaaaaat aaccattctt gctgcacttt atgcaaataa tcaggccaaa tataagacta 300 cagtttattt acaatttgtt tttaccaaaa atgaggacta nagagaaaaa tggtgctcca 360 aagcttatca tacatttgtc attaagtcct agtctc 396 <210> SEQ ID NO 33 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 121, 122, 124, 125, 126, 128, 130, 131, 132, 133, 134, 136, 137, 153, 154, 155, 156, 157, 158, 159, 168, 169, 170, 171, 172, 173, 174, 175, 176, 177, 178, 179, 184, 185, 192, 197, 199, 200, 202, 204, 205, 208, 209, 210, 211, 214, 215 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 216, 217, 218, 222, 227, 228, 229, 233, 234, 241, 242, 244, 245, 246, 247, 248, 249, 252, 260, 261, 262, 263, 264, 265, 270, 272, 273, 274, 275, 279, 282, 284, 288, 290, 291, 292, 293, 294, 299, 300, 301, 302, 303, 306, 313, 314, 319 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 327, 328, 330, 331, 332, 333, 334, 335, 343, 349, 350, 351, 352, 355, 360, 369, 370, 371, 375, 379, 387, 388, 390, 391, 392, 393, 394, 395, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 33 cctttttttt tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt 60 tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt 120 nngnnntntn nnnnannaaa aaaaaaaaaa aannnnnnna aaaaaaannn nnnnnnnnnt 180 tttnnggggg gnttttnann gnannttnnn nttnnnnnaa anccccnnng ggnngggggg 240 nntnnnnnng gnaaaaaaan nnnnnggggn cnnnngggnc cncncccnan nnnnaaaann 300 nnnggntttt ttnnttttna aaaaaanngn nnnnnaacaa aantttttnn nnaanttttn 360 gggggaaann ncccntttnt ttttttnnan nnnnnn 396 <210> SEQ ID NO 34 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 8, 60, 72, 123, 128, 155, 172, 198, 207, 246, 305, 325, 348, 349, 369, 371, 380, 393, 394 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 34 acggaccnag ctggaggagc tgggtgtggg gtgcgttggg ctggtgggga ggcctagttn 60 gggtgcaagt angtctgatt gagcttgtgt tgtgctgaag ggacagccct gggtctaggg 120 ganagagncc ctgagtgtga gacccacctt ccccngtccc agcccctccc anttccccca 180 gggacggcca cttcctgntc cccgacncaa ccatggctga agaacaaccg caggtcgaat 240 tgttcntgaa ggctggcagt gatggggcca agattgggaa ctgcccattc tcccacagac 300 tgttnatggt actgtggctc aaggnagtca ccttcaatgt taccaccnnt gacaccaaaa 360 ggcggaccna nacagtgcan aagctgtgcc canngg 396 <210> SEQ ID NO 35 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 35 tcgaccaaaa tcaaatctgg cactcacaag ccctggccga cccccaatgg gttttaccac 60 tccccctcta gaccctgtct tgcaaaatcc tctccctagc cagctagtat tttctgggct 120 aaagactgta caaccagttc ctccatttta tagaagttta ctcactccag gggaaatggt 180 gagtcctcca acctcccttt caaccagtcc catcattcca accagtggta ccatagagca 240 gcaccccccg ccaccctctg agccagtagt gccagcagtg atgatggcca cccatgagcc 300 cagtgctgac ctggcaccca agaaaaagcc caggaagtca agcatgcctg tgaagattga 360 gaaggaaatt attgataccg ccgatgagtt tgatga 396 <210> SEQ ID NO 36 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 36 tcgacgggaa gagcctgcta cggtggactg tgagactcag tgcactgtcc tcctcccagc 60 gaccccacgc tggaccccct gccggaccct ccacccttcg gcccccaagc ttcccagggg 120 cttcctttgg actggactgt ccctgctcat ccattctcct gccaccccca gacctcctca 180 gctccaggtt gccacctcct ctcgccagag tgatgaggtc ccggcttctg ctctccgtgg 240 cccatctgcc cacaattcgg gagaccacgg aggagatgct gcttgggggt cctggacagg 300 agcccccacc ctctcctagc ctggatgact acgtgaggtc tatatctcga ctggcacagc 360 ccacctctgt gctggacaag gccacggccc agggcc 396 <210> SEQ ID NO 37 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 376 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 37 cgacggtgtc agcaactggc catgccacag cacataaaga ttacagtgac aagaaaaaca 60 ttgtttgagg attcctttca acagataatg agcttcagtc cccaagatct gcgaagacgt 120 ttgtgggtga tttttccagg agaagaaggt ttagattatg gaggtgtagc aagagaatgg 180 ttctttcttt tgtcacatga agtgttgaac ccaatgtatt gcctgtttga atatgcaggg 240 aaggataact actgcttgca gataaacccc gcttcttaca tcaatccaga tcacctgaaa 300 tattttcgtt ttattggcag atttattgcc atggctctgt tccatgggaa aattcataga 360 cacgggtttt tctttnccat tctataagcg tatctt 396 <210> SEQ ID NO 38 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 38 cgaccaaaat gataaatagc tttaagaatg tgctaatgat aaatgattac atgtcaattt 60 aatgtactta atgtttaata ccttatttga ataattacct gaagaatata ttttttagta 120 ctgcatttca ttgattctaa gttgcacttt ttacccccat actgttaaca tatctgaaat 180 cagaatgtgt cttacaatca gtgatcgttt aacattgtga caaagtttaa tggacagttt 240 tttcccatat gtatatataa aataatgtgt tttacaatca gtggcttaga ttcagtgaaa 300 tacagtaatt cattcaatta tgatagtatc tttacagaca ttttaaaaat aagttatttt 360 tatatgctaa tattctatgt tcaagtggaa tttgga 396 <210> SEQ ID NO 39 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 39 tcgaccaaga atagatgctg actgtactcc tcccaggcgc cccttccccc tccaatccca 60 ccaaccctca gagccacccc taaagagata ctttgatatt ttcaacgcag ccctgctttg 120 ggctgccctg gtgctgccac acttcaggct cttctccttt cacaaccttc tgtggctcac 180 agaacccttg gagccaatgg agactgtctc aagagggcac tggtggcccg acagcctggc 240 acagggcaag tgggacaggg catggccagg tggccactcc agacccctgg cttttcactg 300 ctggctgcct tagaaccttt cttacattag cagtttgctt tgtatgcact ttgttttttt 360 ctttgggtct tgtttttttt ttccacttag aaattg 396 <210> SEQ ID NO 40 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 200, 375 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 40 tttttttttt ttttgttatt tagtttttat ttcataatca taaacttaac tctgcaatcc 60 agctaggcat gggagggaac aaggaaaaca tggaacccaa agggaactgc agcgagagca 120 caaagattct aggatactgc gagcaaatgg ggtggagggg tgctctcctg agctacagaa 180 ggaatgatct ggtggttaan ataaaacaca agtcaaactt attcgagttg tccacagtca 240 gcaatggtga tcttcttgct ggtcttgcca ttcctggacc caaagcgctc catggcctcc 300 acaatattca tgccttcttt cactttgcca aacaccacat gcttgccatc caaccactca 360 gtcttggcag tgcanatgaa aaactgggaa ccattt 396 <210> SEQ ID NO 41 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 288 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 41 tcgacctctt gtgtagtcac ttctgattct gacaatcaat caatcaatgg cctagagcac 60 tgactgttaa cacaaacgtc actagcaaag tagcaacagc tttaagtcta aatacaaagc 120 tgttctgtgt gagaattttt taaaaggcta cttgtataat aacccttgtc atttttaatg 180 tacaaaacgc tattaagtgg cttagaattt gaacatttgt ggtctttatt tactttgctt 240 cgtgtgtggg caaagcaaca tcttccctaa atatatatta cccaaagnaa aagcaagaag 300 ccagattagg tttttgacaa aacaaacagg ccaaaagggg gctgacctgg agcagagcat 360 ggtgagaggc aaggcatgag agggcaagtt tgttgt 396 <210> SEQ ID NO 42 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 65, 68, 69, 71, 72, 75, 77, 79, 82, 85, 86, 87, 89, 90, 97, 98, 105, 107, 109, 112, 117, 121, 122, 124, 126, 149, 152, 153, 155, 157, 161, 163, 167, 168, 169, 174, 177, 178, 179, 180, 186, 188, 192, 201, 202, 207, 208, 215, 217, 220 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 225, 230, 242, 243, 247, 250, 259, 263, 271, 272, 279, 284, 295, 298, 299, 308, 309, 312, 323, 342, 348, 351, 363, 366, 370, 386, 390, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 42 cttttttttt tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt 60 aaaanccnna nnaananang gnaannnann aaaaaannca aaccncntnt anaaaangcc 120 nntntnaggg ggggggttca aaaccaaang gnngntngga ngnaaannna aaanttnnnn 180 gggggnanaa anaaaaaggg nngaaanntg acccnanaan gaccngaaan cccgggaaac 240 cnngggntan aaaaaaagnt ganccctaaa nncccccgna aaanggggga agggnaannc 300 caaatccnnt gngggttggg ggnggggaaa aaaaaaaccc cnaaaaantg naaaaaaccg 360 ggnttnaaan atttgggttc gggggntttn tnttaa 396 <210> SEQ ID NO 43 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 108, 195, 213, 279, 287, 349 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 43 tttttttttt ttttgcttca ctgctttatt tttgaaatca caagcaattc aaagtgatca 60 tcattgaggc ttctgttaaa agttcttcca aagttgccca gttttaanat taaacaatat 120 tgcactttaa gatgaactaa cttttgggat tctcttcaaa gaaggaaagt attgctccat 180 ctgtgctttt cttanactaa aagcatactg canaaaactc tattttaaaa atcaacactg 240 cagggtacag taacatagta aagtacctgc ctattttana atcctanaga acatttcatt 300 gtaagaaact agcccattat ttaagtgtcc acagtatttt tcatttcant ggtccaagat 360 gccaaggttt ccaaacacaa tcttgttctc taatac 396 <210> SEQ ID NO 44 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 44 gacctagttt tacctcttaa atatctctgt tcccttctaa gttgtttgct gtgttttctt 60 cagagcaaga aggttatatt ttttaaaatt tacttagtaa tgcacattca aaacacacat 120 caagtcttca ggataaagtt caaaaccgct gtcatggccc catgtgatct ctccctcccc 180 tacccctcta tcatttagtt tcttctgcgc aagccactct ggcttccttt cagttttgtg 240 gttcccgttt ttagctagtt cagtggtttt caatgggcat ttcttgcctt tttttttcta 300 aacgacaaat agaaatacat cttctttatt atcctccaaa tccaattcag aggtaatatg 360 ctccacctac acacaatttt agaaataaat taaaaa 396 <210> SEQ ID NO 45 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 18, 19, 22, 39, 40, 43, 62, 84, 90, 99, 103, 104, 105, 117, 120, 123, 128, 134, 139, 141, 142, 143, 144, 145, 182, 187, 207, 218, 219, 242, 247, 257, 260, 263, 272, 276, 277, 279, 284, 288, 294, 296, 297, 305, 310, 314, 319, 320, 322 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 364, 366, 376, 378, 381, 387, 388, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 45 tttttttttt ttttaaannt tntaaatttt taatgaaann ganttagaac aatgtattat 60 tnacatgtaa ataaaaaaag agancataan ccccatatnc tcnnnaaagg aaggganacn 120 gcnggccntt tatnagaana nnnnncatat aagaccccat taagaagaat ctggatctaa 180 anacttncaa acaggagttc acagtangtg aacagcannc cctaatccca ctgatgtgat 240 gnttcanata aaatcancan cgntgatcgg gnatcnnanc aatntgancg gaanannact 300 gctcnatatn tttnaggann cngatgtggt cattttttac aaagataatg gccacaccct 360 tccngnccga atcgancnga nctcccnntt ctgtgn 396 <210> SEQ ID NO 46 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 24, 105, 144, 188, 190, 214, 317, 369, 371, 378 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 46 tttttttttt tttttttttc tganacagag tctcattctg ttgcctaggc tggattgcag 60 tggtgccatc tcggctcact gcaacctccg cctcctgggt tccanaaatt ctcctgcctc 120 agcctcccgg gtagctggga ctanaggcac acgccaccac gccaggctaa tttttatatt 180 tttagtanan atggcgtttc accatgttga ccanactgat ctcgaactcc cgacctcgtg 240 atccacccac ctcggcctcc caaagtgctg ggattacagg cgtgaaacca ccaggcccgg 300 cctgaaatat ctatttnttt tcagattatt tttaaaattc catttgatga atcttttaaa 360 gtgagctana naaagtgngt gtgtacatgc acacac 396 <210> SEQ ID NO 47 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 290 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 47 tttttttttt tttttttgct gttgccaact gtttattcag ggccctgaac gggtggtgcg 60 tggacatgca acacactcgg gcccacagca gcgtgaccgg ccgctcccaa gccccgggcg 120 cacaaccaca gccaggagca gcccctgcca ccactgggcc accgtccagg gccccacagg 180 accagccgaa ggtgccccgg gccgaggcca gctgggtcag gtgtacccct agcctggggt 240 tgagtgagga gcggcacccc cagtatcctg tgtaccccaa gttgcccagn aggccgaggg 300 ggccttgggc tccatctgca ctggccaccc cgtgccaagc atcacagctg cgtgagcagg 360 tttgtgtgtg agcgtgtggc ggggcctggt tgtccc 396 <210> SEQ ID NO 48 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 393, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 48 ctgggcctgt gccgaagggt ctgggcagat cttccaaaga tgtacaaaat gtagaaattg 60 ccctcaagca aatgcaaaga tgctcaacac ccttagtcat caagaaaatg caaatggaat 120 ccacagagag atactgcaca ctgacaaaga tggtcgtatt actaaaggtg aataaccagc 180 gcggggggca cgtggagtca ctggaacatt tgtgcaatgc tggtgggaat gtcaacccgt 240 gcggccctct ggaataagcc tggcagctcc tccaagagtt acccgtgtga cccagcaatt 300 ccactcctag ctccacccac aggaattgaa agcaaagacg caaacagatg cctgtgcacc 360 aaagttcacg gcagcatcct tcgccatagt ggnaan 396 <210> SEQ ID NO 49 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 32, 40, 44, 64, 70, 83, 87, 92, 104, 115, 118, 125, 127, 130, 137, 155, 168, 171, 173, 175, 192, 201, 206, 208, 218, 219, 235, 247, 249, 256, 259, 260, 269, 297, 306, 310, 320, 321, 328, 331, 345, 356, 381, 389, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 49 accccaaaat gggaaaggaa aagactcata tnaacattgn cgtnattgga cacgtacatt 60 cggncaagtn caccactact ggncatntga tntataaatg cggnggcatc gacanaanaa 120 ccatngnaan atttganaag gaggctgctg atatnggaaa gggctccntc nantntgcct 180 gggtcttgga tnaactgaaa nctgancntg aacgtggnnt caccattgat atctncttgt 240 ggaaatntna gaccancann tactatgtna ctatcattga tgccccagga cacaganact 300 ttatcnaaan catgattacn nggacatnta nagctgactg tgctngcctg attgtngctg 360 ctggtgttgg tgaatttgaa nctggtatnt ccaana 396 <210> SEQ ID NO 50 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 50 cgacttcttg ctggtgggtg gggcagtttg gtttagtgtt atactttggt ctaagtattt 60 gagttaaact gcttttttgc taatgagtgg gctggttgtt agcaggtttg tttttcctgc 120 tgttgattgt tactagtggc attaactttt agaatttggg ctggtgagat taattttttt 180 taatatccca gctagagata tggcctttaa ctgacctaaa gaggtgtgtt gtgatttaat 240 tttttcccgt tcctttttct tcagtaaacc caacaatagt ctaaccttaa aaattgagtt 300 gatgtcctta taggtcacta cccctaaata aacctgaagc aggtgttttc tcttggacat 360 actaaaaaat acctaaaagg aagcttagat gggctg 396 <210> SEQ ID NO 51 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 18, 52, 59, 148, 267, 321, 332 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 51 tttttttttt ttcagcgngg atttatttta tttcattttt tactctcaag anaaagaana 60 gttactattg caggaacaga cattttttta aaaagcgaaa ctcctgacac ccttaaaaca 120 gaaaacattg ttattcacat aataatgngg ggctctgtct ctgccgacag gggctgggtt 180 cgggcattag ctgtgccgtc gacaatagcc ccattcaccc cattcataaa tgctgctgct 240 acaggaaggg aacagcggct ctcccanaga gggatccacc ctggaacacg agtcacctcc 300 aaagagctgc gactgtttga naatctgcca anaggaaaac cactcaatgg gacctggata 360 acccaggccc gggagtcata gcaggatgtg gtactt 396 <210> SEQ ID NO 52 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 81, 189 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 52 acctcgctaa gtgttcgcta cgcggggcta ccggatcggt cggaaatggc agaggtggag 60 gagacactga agcgactgca nagccagaag ggagtgcagg gaatcatcgt cgtgaacaca 120 gaaggcattc ccatcaagag caccatggac aaccccacca ccacccagta tgccagcctc 180 atgcacagnt tcatcctgaa ggcacggagc accgtgcgtg acatcgaccc ccagaacgat 240 ctcaccttcc ttcgaattcg ctccaagaaa aatgaaatta tggttgcacc agataaagac 300 tatttcctga ttgtgattca gaatccaacc gaataagcca ctctcttggc tccctgtgtc 360 attccttaat ttaatgcccc ccaagaatgt taatgt 396 <210> SEQ ID NO 53 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 224, 225, 228, 235, 240, 246, 257, 266, 274, 279, 281, 282, 283, 285, 287, 288, 290, 291, 292, 293, 294, 295, 296, 297, 300, 301, 303, 307, 311, 313, 314, 317, 318, 319, 320, 321, 323, 324, 328, 329, 330, 336, 337, 338, 339, 340, 341 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 342, 343, 344, 345, 346, 347, 348, 349, 350, 351, 352, 356, 357, 358, 359, 362, 363, 364, 365, 366, 367, 373, 380, 381, 382, 385, 387, 388, 389, 390, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 53 tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt 60 tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt 120 tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt tttttttttt 180 tttttttttt tttttttttt tttttttttt tttttttttt ttannttntt ttttnttttn 240 cctttntttt aattcanaaa aagaanaaga aaanataana nnnancnnan nnnnnnnatn 300 ntncttnata ntnnttnnnn nanngggnnn gcgagnnnnn nnnnnnnnnn nntctnnnnt 360 tnnnnnnctt gcnccccttn nnttngnnnn angcaa 396 <210> SEQ ID NO 54 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 367 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 54 ctcttggggc tgctgggact cgcgtcggtt ggcgactccc ggacgtaggt agtttgttgg 60 gccgggttct gaggccttgc ttctctttac ttttccactc taggccacga tgccgcagta 120 ccagacctgg gaggagttca gccgcgctgc cgagaagctt tacctcgctg accctatgaa 180 ggcacgtgtg gttctcaaat ataggcattc tgatgggaac ttgtgtgtta aagtaacaga 240 tgatttagtt tgtttggtgt ataaaacaga ccaagctcaa gatgtaaaga agattgagaa 300 attccacagt caactaatgc gacttatggt agccaaggaa gcccgcaatg ttaccatgga 360 aactgantga atggtttgaa atgaagactt tgtcgt 396 <210> SEQ ID NO 55 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 55 cgacggtttg ccgccagaac acaggtgtcg tgaaaactac ccctaaaagc caaaatggga 60 aaggaaaaga ctcatatcaa cattgtcgtc attggacacg tagattcggg caagtccacc 120 actactggcc atctgatcta taaatgcggt ggcatcgaca aaagaaccat tgaaaaattt 180 gagaaggagg ctgctgagat gggaaagggc tccttcaagt atgcctgggt cttggataaa 240 ctgaaagctg agcgtgaacg tggtatcacc attgatatct ccttgtggaa atttgagacc 300 agcaagtact atgtgactat cattgatgcc ccaggacaca gagactttat caaaaacatg 360 attacaggga catctcaggc tgactgtgct gtcctg 396 <210> SEQ ID NO 56 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 134, 145, 255, 279, 337, 344, 369 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 56 tttttttttt ttttttctca tttaactttt ttaatgggtc tcaaaattct gtgacaaatt 60 tttggtcaag ttgtttccat taaaaagtac tgattttaaa aactaataac ttaaaactgc 120 cacacgcaaa aaanaaaacc aaagnggtcc acaaaacatt ctcctttcct tctgaaggtt 180 ttacgatgca ttgttatcat taaccagtct tttactacta aacttaaatg gccaattgaa 240 acaaacagtt ctganaccgt tcttccacca ctgattaana gtggggtggc aggtattagg 300 gataatattc atttagcctt ctgagctttc tgggcanact tggngacctt gccagctcca 360 gcagccttnt tgtccactgc tttgatgaca cccacc 396 <210> SEQ ID NO 57 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 52, 57, 58, 61, 72, 75, 77, 84, 87, 88, 93, 100, 101, 111, 117, 119, 121, 131, 132, 133, 134, 142, 143, 154, 156, 159, 167, 168, 170, 175, 176, 182, 183, 185, 186, 190, 192, 194, 198, 199, 200, 209, 212, 217, 218, 220, 232, 235, 253 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 255, 257, 258, 260, 262, 263, 270, 271, 273, 277, 280, 281, 284, 285, 289, 296, 297, 298, 303, 305, 307, 309, 310, 317, 322, 324, 337, 338, 342, 344, 346, 347, 349, 351, 356, 358, 366, 368, 371, 377, 380, 388, 389, 393, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 57 cctttttttt tttttttttt tttttttttt tttttttttt tttttttttt tnaaaanntt 60 ntttttgcaa anccnancaa aaanggnngg aangaaaaan nggaaaaatt ntttttncnt 120 ntttgggaac nnnnagccct tnntttgaaa aaangnggnc ttaaaanngn tgaannaaag 180 gnnanncccn gntncttnnn tttaaaaana anggggnngn ttttttttaa anaanatttt 240 ttttttccct aanancnncn anntgaaacn ngncccnacn nctnncttna aagggnnnaa 300 atnanangnn aaaaaanccc tnancccccc cccttanntt tncnannana naaagncntt 360 ttgggncntg naaaaanaan cctttttnnt gcnttn 396 <210> SEQ ID NO 58 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 58 cgacctcaaa tatgccttat tttgcacaaa agactgccaa ggacatgacc agcagctggc 60 tacagcctcg atttatattt ctgtttgtgg tgaactgatt ttttttaaac caaagtttag 120 aaagaggttt ttgaaatgcc tatggtttct ttgaatggta aacttgagca tcttttcact 180 ttccagtagt cagcaaagag cagtttgaat tttcttgtcg cttcctatca aaatattcag 240 agactcgagc acagcaccca gacttcatgc gcccgtggaa tgctcaccac atgttggtcg 300 aagcggccga ccactgactt tgtgacttag gcggctgtgt tgcctatgta gagaacacgc 360 ttcaccccca ctccccgtac agtgcgcaca ggcttt 396 <210> SEQ ID NO 59 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 25, 45, 116, 178, 198, 211, 225, 235, 253, 266, 281, 324, 367, 377, 389 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 59 cttttttttt tttttttttt tcagnggaaa ataactttta ttganacccc accaactgca 60 aaatctgttc ctggcattaa gctccttctt cctttgcaat tcggtctttc ttcagnggtc 120 ccatgaatgc tttcttctcc tccatggtct ggaagcggcc atggccaaac ttggaggngg 180 tgtcaatgaa cttaaggnca atcttctcca nagcccgccg cttcntctgc accancaagg 240 acttgcggag ggngagcacc cgcttnttgg ttcccaccac ncagcctttc agcatgacaa 300 agtcattggt cacttcacca tagnggacaa agccacccaa agggttgatg ctccttggca 360 aataggncat agtcacngga ggcattgtnc ttgatc 396 <210> SEQ ID NO 60 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 60 acctcagctc tcggcgcacg gcccagcttc cttcaaaatg tctactgttc acgaaatcct 60 gtgcaagctc agcttggagg gtgatcactc tacaccccca agtgcatatg ggtctgtcaa 120 agcctatact aactttgatg ctgagcggga tgctttgaac attgaaacag ccatcaagac 180 caaaggtgtg gatgaggtca ccattgtcaa cattttgacc aaccgcagca atgcacagag 240 acaggatatt gccttcgcct accagagaag gaccaaaaag gaacttgcat cagcactgaa 300 gtcagcctta tctggccacc tggagacggt gattttgggc ctattgaaga cacctgctca 360 gtatgacgct tctgagctaa aagcttccat gaaggg 396 <210> SEQ ID NO 61 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 61 tagcttgtcg gggacggtaa ccgggacccg gtgtctgctc ctgtcgcctt cgcctcctaa 60 tccctagcca ctatgcgtga gtgcatctcc atccacgttg gccaggctgg tgtccagatt 120 ggcaatgcct gctgggagct ctactgcctg gaacacggca tccagcccga tggccagatg 180 ccaagtgaca agaccattgg gggaggagat gactccttca acaccttctt cagtgagacg 240 ggcgctggca agcacgtgcc ccgggctgtg tttgtagact tggaacccac agtcattgat 300 gaagttcgca ctggcaccta ccgccagctc ttccaccctg agcagctcat cacaggcaag 360 gaagatgctg ccaataacta tgcccgaggg cactac 396 <210> SEQ ID NO 62 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 261, 269, 313, 333, 346, 354, 359, 390, 394, 395, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 62 tcgacgtttc ctaaagaaaa ccactctttg atcatggctc tctctgccag aattgtgtgc 60 actctgtaac atctttgtgg tagtcctgtt ttcctaataa ctttgttact gtgctgtgaa 120 agattacaga tttgaacatg tagtgtacgt gctgttgagt tgtgaactgg tgggccgtat 180 gtaacagctg accaacgtga agatactggt acttgatagc ctcttaagga aaatttgctt 240 ccaaatttta agctggaaag ncactggant aactttaaaa aagaattaca atacatggct 300 ttttagaatt tcnttacgta tgttaagatt tgngtacaaa ttgaantgtc tgtnctganc 360 ctcaaccaat aaaatctcag tttatgaaan aaannn 396 <210> SEQ ID NO 63 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 3, 11, 16, 18, 23, 26, 30, 34, 37, 50, 51, 60, 61, 62, 63, 64, 75, 82, 83, 84, 85, 87, 89, 93, 94, 97, 98, 99, 118, 119, 120, 122, 134, 136, 138, 139, 141, 144, 145, 147, 152, 156, 187, 188, 193, 195, 204, 211, 214, 216, 222, 226 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 228, 235, 242, 258, 264, 265, 269, 275, 294, 298, 301, 307, 316, 326, 334, 335, 339, 340, 343, 350, 351, 355, 373, 378, 390 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 63 ttnttttttt nttttntntt ttntcnttgn ttgnacngaa cccggcgctn nttccccacn 60 nnnnacggcc gcccntattc annnntncnt canntannna ccgcaccctc ggactgcnnn 120 tngggccccg ccgncnannc nccnncnccc anttcnccgc cgccgccgcc gccttttttt 180 attggcnncc atnanaaccg gggncacctc ncangngcgc cnaaantngg ggcangactc 240 anagggggcc atcaaccncc aagnncaanc tgganctcta caaacggcct acgntttntg 300 nccatgnggg tagggnttta cccgcnatga tgannatgnn aanaactttn ncaanccctt 360 tattaaccaa tgnggtgngg agacggaacn tggtta 396 <210> SEQ ID NO 64 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 175, 177, 340, 393 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 64 tcgacgtcgg ggtttcctgc ttcaacagtg cttggacgga acccggcgct cgttccccac 60 cccggccggc cgcccatagc cagccctccg tcacctcttc accgcaccct cggactgccc 120 caaggccccc gccgccgctc cagcgccgcg cagccaccgc cgccgccgcc gcctntnctt 180 agtcgccgcc atgacgaccg cgtccacctc gcaggtgcgc cagaactacc accaggactc 240 agaggccgcc atcaaccgcc agatcaacct ggagctctac gcctcctacg tttacctgtc 300 catgtcttac tactttgacc gcgatgatgt ggctttgaan aactttgcca aatactttct 360 tcccaatctc atgaggagaa ggaacatgct ganaaa 396 <210> SEQ ID NO 65 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 26, 56, 103, 122, 145, 151, 154, 187, 189, 203, 224, 256, 273, 305, 344 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 65 tttttttttt tttttttttt tttttnacca ataatgcttt tattttccac atcaanatta 60 atttatatgt tagttttagt acaagtacta aaatgtatac ttnttgccct aatagctaag 120 gnatacataa gcttcaccat acatnttgca nccncctgtc tgtcctatgt cattgttata 180 aatgtanana ttttaggaaa ctnttttatt caacctggga catntatact gtaggagtta 240 gcactgacct gatgtnttat ttaaaagtaa tgnatattac ctttacatat attccttata 300 tattnaaacg tatttccatg ttatccagct taaaatcaca tggnggttaa aagcatgagt 360 tctgagtcaa atctggactg aaatcctgat gctccc 396 <210> SEQ ID NO 66 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 66 tcgacttttt tttttccagg acattgtcat aattttttat tatgtatcaa attgtcttca 60 atataagtta caacttgatt aaagttgata gacatttgta tctatttaaa gacaaaaaaa 120 ttcttttatg tacaatatct tgtctagagt ctagcaaata tagtaccttt cattgcagga 180 tttctgctta atataacaag caaaaacaaa caactgaaaa aatataaacc aaagcaaacc 240 aaaccccccg ctcaactaca aatgtcaata ttgaatgaag cattaaaaga caaacataaa 300 gtaacttcag cttttatcta gcaatgcaga atgaatacta aaattagtgg caaaaaaaca 360 aacaacaaac aacaaacaaa acaaaacaaa caaaca 396 <210> SEQ ID NO 67 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 67 acgcttttgt ccttcatttt aactgttatg tcatactgtt atgttgacat atttctttat 60 aagagaatag aggcaaaagt atagaactga ggatcatttg tatttttgag ttggaaatta 120 tgaaacttca ccatattatg atcatacata ttttgaagaa cagactgacc aaagctcacc 180 tgttttttgt gttaggtgct ttggctgaac ttgattccag cccccttttc cctttggtgt 240 tgtgtatgtc tcttcatttc ctctcaaatc ttcaactctt gccccatgtc tccttggcag 300 caggatgctg gcatctgtgt agtcctcata ctgtttactg ataacccaca aattcatttt 360 catggcagac ctaagctcag accctgcctt gtcctg 396 <210> SEQ ID NO 68 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 68 acctgagtcc tgtcctttct ctctccccgg acagcatgag cttcaccact cgctccacct 60 tctccaccaa ctaccggtcc ctgggctctg tccaggcgcc cagctacggc gcccggccgg 120 tcagcagcgc ggccagcgtc tatgcaggcg ctgggggctc tggttcccgg atctccgtgt 180 cccgctccac cagcttcagg ggcggcatgg ggtccggggg cctggccacc gggatagccg 240 ggggtctggc aggaatggga ggcatccaga acgagaagga gaccatgcaa agcctgaacg 300 accgcctggc ctcttacctg gacagagtga ggagcctgga gaccgagaac cggaggctgg 360 agagcaaaat ccgggagcac ttggagaaga agggac 396 <210> SEQ ID NO 69 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1, 4, 6, 8, 9, 11, 18, 19, 36, 53, 60, 64, 79, 84, 92, 94, 97, 105, 114, 120, 123, 127, 129, 134, 137, 138, 139, 142, 143, 147, 149, 151, 152, 156, 158, 167, 170, 172, 180, 182, 184, 187, 188, 189, 194, 197, 201, 209, 212, 218, 219 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 220, 222, 223, 225, 228, 229, 230, 232, 233, 236, 242, 244, 247, 250, 251, 253, 256, 257, 259, 261, 270, 271, 274, 277, 278, 279, 282, 284, 288, 289, 296, 298, 300, 310, 315, 316, 320, 321, 324, 328, 330, 331, 334, 336, 340, 347, 350 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 352, 353, 355, 359, 361, 362, 364, 367, 370, 372, 374, 376, 382, 388, 390, 394, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 69 ntcncngnng ntgtggtnnt ttttttaatt tttatntttt cttttttttt ctngctagcn 60 cttncttttt ttggaattnc ggtncctttt tntntcnatt ttttngacaa aaanaacctn 120 ttntttnana ccanagnnng gnncacncnt nnaatntncc ccttttncgn tngggagctn 180 cncnttnnnc gccnacntca ntcgagacng tncttttnnn tnnancannn tnngtncgtt 240 gncngcnttn ntncannant nttccctatn nacntgnnnt cncncatnnt tggacnancn 300 cctagccttn ccatnntttn nttntttntn natnancctn gaaaacntcn gnntnttcnc 360 nncnttnccn cncncncctt cntatgtncn atgncn 396 <210> SEQ ID NO 70 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 15, 38, 57, 59, 63, 64, 65, 66, 68, 78, 79, 84, 87, 90, 97, 114, 115, 127, 128, 141, 143, 145, 151, 159, 168, 169, 172, 173, 176, 178, 197, 198, 207, 209, 211, 215, 220, 221, 223, 225, 228, 240, 248, 249, 260, 262, 263, 273, 283, 287 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 294, 304, 314, 334, 339, 340, 348, 362, 367, 376, 382, 384, 386, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 70 tttttttttt ttttnttttt tttttttttt tttttttntt tttttttttt ttttttntnc 60 aannnntnaa cttttaanng gccnccngcn ccccaanggg gaccctgctt ttgnnggcta 120 aatgccnnaa aactttgggg nantnggtat naaaccccnc tttgcccnnc annttncngg 180 gggggggggg tttttgnngg ggaacangna naacnttttn ncnanggnat caccaaaaan 240 aaagcccnnc cctttttccn annggggggg ggngggggga aantcanccc ccanattgac 300 cttnatttca aaanggggct tataatcctg ggcntggann cttccctnta cccgggggtt 360 gnccacnttt tattanaggg gnangnggat ccccnt 396 <210> SEQ ID NO 71 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 15, 21, 30, 33, 35, 36, 42, 43, 44, 45, 46, 51, 56, 58, 59, 63, 70, 77, 81, 88, 94, 95, 96, 97, 101, 102, 109, 114, 118, 119, 120, 124, 131, 132, 133, 134, 135, 141, 142, 143, 144, 145, 146, 148, 149, 154, 158, 162, 164, 166, 172 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 177, 179, 181, 184, 185, 213, 216, 218, 219, 222, 223, 224, 230, 231, 240, 241, 242, 245, 247, 251, 252, 255, 258, 259, 261, 264, 268, 269, 272, 276, 285, 288, 289, 291, 292, 293, 297, 299, 300, 307, 312, 315, 316, 317, 325, 329, 334 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 340, 341, 347, 350, 354, 355, 357, 360, 361, 367, 368, 370, 371, 376, 377, 378, 387, 393, 394 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 71 gcatctagag ggccngttta ntctagaggn ccngnntaaa cnnnnncatc nacctncnnt 60 gcncctgctn gttgccnccc ntctgtgnct tgcnnnnccc nngagcgtnc cttnaccnnn 120 gaangtgcct nnnnnactga nnnnnncnna taanatgngg anantncgtc gncattntnt 180 natnnggggt gatgctattc tggggggtgg ggnggngnna tnnnatactn nggggacgtn 240 nnatnangag nnatntcnng nttntctnnt gntttntggg gggcnatnng nnntctntnn 300 ggactcntcg cncannnatc aatancttna ttcngtgtan ngtccgnccn tagnncngcn 360 ngtactnnan ngttgnnntc attactnttc gtnngg 396 <210> SEQ ID NO 72 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 2, 23, 27, 34, 35, 36, 37, 39, 41, 45, 55, 56, 59, 61, 88, 92, 96, 97, 98, 101, 103, 104, 106, 108, 111, 114, 115, 121, 128, 129, 131, 159, 170, 191, 202, 227, 233, 235, 240, 262, 268, 271, 272, 280, 281, 303, 304, 305, 311, 316, 317 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 321, 324, 336, 344, 345, 353, 360, 362, 363, 364, 365, 366, 370, 373, 389, 391, 392, 394, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 72 tntttttttt tttctaaaac atnactnttt attnnnnang ntttntgaac ctctnngcnt 60 natggtgaga gtttgtctga ttaataanaa tnggannntt nannanangc ntgnncgcaa 120 ngatggcnnc nctgtatatc ccaccatccc attacactnt gaaccttttn tttgattaat 180 aaaaggaagg natgcgggga anggggaaag agaatgcttg aacattncca tgngnccttn 240 gacaaacttt ccaatggagg cnggaacnaa nnaccaccan ncaactcccc tttttgtaat 300 ttnnnaactt ncaacnncta nctntttatt ttggcntccc tggnngaaac agnctgtatn 360 annnnnaagn ccntgagaac atccctggnt nncnna 396 <210> SEQ ID NO 73 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1, 7, 9, 14, 23, 35, 38, 44, 48, 50, 61, 74, 76, 79, 80, 85, 86, 91, 95, 101, 109, 112, 113, 117, 118, 121, 122, 127, 129, 132, 137, 141, 146, 214, 234, 243, 251, 266, 296, 305, 306, 336 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 73 ntcaacntng actnctgtga ggnatggtgc tgggngcnta tgcngtgngn ttttggatac 60 naccttatgg acantngcnn tcccnnggaa ngatnataat ncttactgna gnnactnnaa 120 nnttccntnt cnaaaangtt naaaancatt ggatgtgcca caatgatgac agtttatttg 180 ctactcttga gtgctataat gatgaagatc ttanccacca ttatcttaac tgangcaccc 240 aanatggtga nttggggaac atatanagta cacctaagtt cacatgaagt tgtttnttcc 300 caggnnctaa agagcaagcc taactcaagc cattgncaca caggtgagac acctctattt 360 tgtacttctc acttttaagg gattagaaaa tagcca 396 <210> SEQ ID NO 74 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 22, 118 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 74 cctttttttt tttttttact gngaatatat actttttatt tagtcatttt tgtttacaat 60 tgaaactctg ggaattcaaa attaacatcc ttgcccgtga gcttcttata gacaccanaa 120 aaagtttcaa ccttgtgttc cacattgttc tgctgtgctt tgtccaaatg aacctttatg 180 agccggctgc catctagttt gacgcggatt ctcttgccca caatttcgct tgggaagacc 240 aagtcctcaa ggatggcatc gtgcacagct gtcagagtac ggctcctggg acgcttttgc 300 ttattttttg tacggctttt tcgagttggc ttaggcagaa ttctcctctg agcgataaag 360 acgacatgct tcccactgaa ctttttctcc aattcg 396 <210> SEQ ID NO 75 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 14, 38, 41, 43, 47, 53, 73, 75, 78, 83, 96, 112, 113, 117, 124, 127, 146, 160, 167, 169, 176, 177, 178, 179, 194, 197, 198, 209, 210, 220, 222, 226, 227, 231, 238, 241, 244, 258, 259, 260, 270, 271, 274, 288, 301, 302, 305, 307, 316 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 319, 328, 339, 344, 347, 354, 359, 364, 367, 369, 370, 371, 373, 374, 381, 384, 387, 388 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 75 tttttttttt tttntttttt tttttttttt tttttttnaa ntntaanggg ganggcccct 60 tttttttaaa ctngnccntt ttnctttcct tttttnaaaa ggaaaaaaaa anntttnttt 120 ttcnttnaaa aacccttttt cccacnaaca aaaaaaaccn ttccccntnc cttttnnnna 180 aaaaaaaggg gctnggnntt tccccttann caaaaaaccn tntccnnggg naaaaaantt 240 ntcnccgggg gggaaacnnn tgggggtgtn nccnaaattt gggggccntc ggaagggggg 300 nnccncncct aaagangtnt ttcaaaanaa aaacccccnt cctnttntaa aaanaaaana 360 aaanaangnn ngnntttttt ntcnttnncc ccccaa 396 <210> SEQ ID NO 76 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 87, 94, 102, 108, 138, 139, 143, 144, 145, 146, 151, 152, 158, 168, 170, 171, 187, 204, 206, 224, 261, 262, 267, 268, 270, 287, 305, 306, 313, 315, 319, 320, 330, 331, 333, 342, 344, 348, 349, 356, 358, 360, 362, 368, 374, 376, 381 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 390 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 76 acattcttca gaaatacagt gatgaaaatt cattttgaaa ctcaaatatt ttcattttgg 60 atattctcct gtttttatta aaccagngat tacncctggc cntccctnta aatgttctag 120 gaaggcatgt ctgttgtnnt ttnnnnaaaa nnaaattntt tttttttngn naaaccccaa 180 atcccanttt atcaggaagt tagncnaatg aaatggaaat tggntaatgg acaaaagcta 240 gcttgtaaaa aggaccaccc nnccacnngn ctttaccccc ttggttngtt gggggaaaaa 300 ccatnnttaa ccntntggnn aaaattgggn ncntaaagtt tncntggnna acagtncntn 360 cngtattnaa ttgncnttat nggaaaatcn gggatt 396 <210> SEQ ID NO 77 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 63, 66, 81, 83, 89, 107, 115, 118, 147, 151, 190, 232, 275, 288, 294, 304, 323, 332, 369, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 77 tttttttttt tttttttttt tttttttttt tatcaacatt tatatgcttt attgaaagtt 60 ganaanggca acagttaaat ncngggacnc cttacaattg tgtaaanaac atgcncanaa 120 acatatgcat ataactacta tacaggngat ntgcaaaaac ccctactggg aaatccattt 180 cattagttan aactgagcat ttttcaaagt attcaaccag ctcaattgaa anacttcagt 240 gaacaaggat ttacttcagc gtattcagca gctanatttc aaattacnca aagngagtaa 300 ctgngccaaa ttcttaaaat ttntttaggg gnggtttttg gcatgtacca gtttttatgt 360 aaatctatnt ataaaagtcc acacctcctc anacag 396 <210> SEQ ID NO 78 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 8, 14, 16, 20, 26, 28, 36, 38, 39, 40, 51, 52, 55, 57, 58, 67, 71, 114, 120, 132, 138, 142, 159, 165, 169, 172, 174, 175, 183, 187, 195, 197, 198, 200, 202, 206, 209, 243, 259, 260, 267, 283, 292, 305, 311, 315, 317, 319, 323, 324 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 331, 333, 334, 338, 343, 348, 353, 355, 357, 366, 376, 388 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 78 agctggcnaa aggngnatgn gctgcnangc gattangnnn ggtaacgtca nnggntnncc 60 agtgcangac nttgtaaaac gacggccaca tgaattgtaa tacgactcac tatngggcgn 120 attgggccgt gnaggatngt gntcacactc gaatgtatnc tggcngatnc ananngcttt 180 atngctnttg acggngnntn anccanctng ggctttaggg ggtatcccct cgcccctgct 240 tcnttgattt gcacgggcnn ctccganttc cttcataata ccngacgctt cnatccccta 300 gctcngacct ntcantntnt tcnntgggtt ntnnccgntc acngcttncc cgnangntat 360 aatctnggct cctttnggga tccattantc tttact 396 <210> SEQ ID NO 79 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 116, 153, 189, 194, 210, 218, 241, 270, 272, 288, 291, 304, 324, 325, 329, 333, 334, 338, 340, 342, 366, 372, 377, 384, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 79 caccaaccaa aacctggcgc cgttggcatc gtagagtgaa cacaacccaa aaacgatacg 60 ccatctgttc tgccctggct gcctcagccc taccagcact ggtcatgtct aaaggncatc 120 gtattgagga agttcctgaa cttcctttgg tangttgaag ataaagctga aggctacaag 180 aagaccaang aagntgtttt gctccttaan aaacttanac gcctggaatg atatcaaaaa 240 ngctatgcct ctcagcgaat gagactggan angcaaaatg agaaaccntc nccgcatcca 300 gcgnaggggc cgtgcatctc tatnntgang atnntggnan cnttcaaggc cttcagaacc 360 tccctngaaa tnctctnctt taangaacca aactgn 396 <210> SEQ ID NO 80 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 312, 319, 353, 383 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 80 tgtacatagg catcttattc actgcaccct gtcacaccca gcaccccccg ccccgcacat 60 tatttgaaag actgggaatt taatggttag ggacagtaaa tctacttctt tttccaggga 120 cgactgtccc ctctaaagtt aaagtcaata caagaaaact gtctattttt agcctaaagt 180 aaaggctgtg aagaaaattc attttacatt gggtagacag taaaaaacaa gtaaaataac 240 ttgacatgag cacctttaga tccttccctt catggggctt tgggcccaga atgacctttg 300 aggcctgtaa anggattgna atttcctata agctgtatag tggagggatt ggngggtcat 360 ttgagtaagc cctccaagat acnttcaata cctggg 396 <210> SEQ ID NO 81 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 240, 286, 361, 364, 374, 375, 379, 380, 381, 387 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 81 gcagctgaag ttcagcaggt gctgaatcga ttctcctcgg cccctctcat tccacttcca 60 acccctccca ttattccagt actacctcag caatttgtgc cccctacaaa tgttagagac 120 tgtatacgcc ttcgaggtct tccctatgca gccacaattg aggacatcct gcatttcctg 180 ggggagttcg ccacagatat tcgtactcat ggggttcaca tggttttgaa tcaccagggn 240 ccgccatcag gagatgcctt tatccagatg aagtctgcgg acagancatt tatggctgca 300 cagaagtggc ataaaaaaaa catgaaggac agatatgttg aagttttcag tgtcagctga 360 nganagaaca ttgnngtann ngggggnact ttaaat 396 <210> SEQ ID NO 82 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 220, 251, 297, 301, 309, 349, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 82 gactcagaaa tgtcagtctc atgaagttca aaagatcgag aatgtttgct atcttggtgg 60 agcagccgca gccaagcaag taacttgtaa aatgaggaat gccatcaccc ctcgagtgtc 120 catcccacat aacttggggt tagagcacaa gcgttcccag gaactactca ccttaccatc 180 ttggccgttt catttgcttc caccagttct ggaaagagan ggcctagaag ttcaaaaaaa 240 aagtaggaaa ngtgcttttg gagaaaatca cctgctcctc agaactgggc ttacaanctg 300 ngaagtacnc tatgtgccac ctaatcctca tatatgacct caagagacnc caataagcat 360 atttccacca cggaatgacc agtgctttgg gtaana 396 <210> SEQ ID NO 83 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 13, 372, 379, 393 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 83 tttgatttaa ganatttatt atttttttaa aaaaagcaac ttccagggtt gtcattgtac 60 aggttttgcc cagtctccta tagcatggta tagtgataac tgatttttta taacaatgac 120 tcagaggcat tgaagatcca taactatctt ctgaattatc acagaaagaa gaaagttaga 180 agagtttaat gttaagtgta ttaaaaatca tattctaatt cttttaattt ggttatctga 240 gtatgataat ataggagagc tcagataaca aggaaaaggc attggggtaa gaacactcct 300 tcccacagga tggcattaac agactttttc tgcatatgct ttatatagtt gccaactaat 360 tcacctttta cncagcttna ttttttttta ctnggg 396 <210> SEQ ID NO 84 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 61, 232, 254, 270, 271, 286, 354, 356, 368, 374, 389, 394 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 84 tttttacagc aatttttttt tattgatgtt taacctgtat acaaccatac ccattttaag 60 ngtacagaca aatgaatttt gacaaattca ttcactcatc taatcatcac tataaccatg 120 atacagattt ttatcactcc aaaagtccat cctgtgctct tttcaagtcc atcctcctca 180 tctgataccc caagccacca ttgttttgct ttctggaact acagttttgg gnttttagaa 240 tttcatatat ggtngaatca taccatttgn natttggggc tgacgncttt cctccaataa 300 tggatttgag aattatctac attttgcatg gatcctgggt tatttatacc aacnangggt 360 tattatgnaa aatnggacca caatttggng gcanta 396 <210> SEQ ID NO 85 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 293, 305, 306, 317, 347, 357, 372, 377, 386, 391 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 85 cagtgaccgt gctcctaccc agctctgctc cacagcgccc acctgtctcc gcccctcggc 60 ccctcgcccg gctttgccta accgccacga tgatgttctc gggcttcaac gcagactacg 120 aggcgtcatc ctcccgctgc agcagcgcgt ccccggccgg ggatagcctc tcttactacc 180 actcacccgc agactccttc tccagcatgg gctcgcctgc aacgcgcagg acttctgcac 240 ggacctggcc gctccagtgc caacttcatt ccacggcact gcatctcgac canccggact 300 tgcannggtt ggggaanccg cccttgtttc tccgtggccc atctaanacc aaacccntca 360 ccttttcgga gnccccnccc ctccgntggg nttact 396 <210> SEQ ID NO 86 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 5, 6, 28, 50, 58, 90, 108, 110, 118, 145, 154, 194, 244, 285, 292, 300, 312, 315, 342, 344, 346, 359, 374, 378, 380, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 86 ttttnnactg aatgtttaat acatttgnag gaacagaaga aatgcagtan ggattaanat 60 tttataatta gacattaatg taacagatgn ttcatttttc aaagaagntn cccccttntc 120 cctatctttt tttaatcttc cttanagcaa taantagtaa ttactatatt tgtggacaag 180 ctgctccact gtgntggaca gtaattatta aatctttatg tttcacatca ttattacctt 240 ccanaattct accttcattt ccctgcacag gttcactgga ctggntcaca ancaaattgn 300 actccactca antanaagag cccaaagaaa ttagagtaac gncnantcct atgaattana 360 gacccaaaga tttnaggngn tgattagaaa cataan 396 <210> SEQ ID NO 87 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 231, 277, 285, 296, 341, 351, 372, 377, 380 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 87 atggaggcgc tggggaagct gaagcagttc gatgcctacc ccaagacttt ggaggacttc 60 cgggtcaaga cctgcggggg cgccaccgtg accattgtca gtggccttct catgctgcta 120 ctgttcctgt ccgagctgca gtattacctc accacggagg tgcatcctga gctctacgtg 180 gacaagtcgc ggggagataa actgaagatc aacatcgatg tactttttcc ncacatgcct 240 tgtgcctatc tgagtattga tgccatggat gtggccngag aacancagct ggatgnggaa 300 cacaacctgt ttaagccacc actagataaa gatgcatccc ngtgagctca nagctgagcg 360 gcatgagctt gngaaantcn aggtgaccgg gtttga 396 <210> SEQ ID NO 88 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 246, 266, 301, 328, 347, 349, 368, 370, 371, 374, 379, 387, 391 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 88 tccagagcag agtcagccag catgaccgag cgccgcgtcc ccttctcgct cctgcggggc 60 cccagctggg accccttccg cgactggtac ccgcatagcc gctcttcgac caggccttcg 120 ggctgccccg gctgccggag gagtggtcgc agtggttagg cggcagcagc tggccaggct 180 acgtgcgccc cctgcccccc gccgcatcga gagccccgca gtggccgcgc ccgctacagc 240 cgcgcngctc agccggcaac tcacancggg gctcggagat ccgggacact gcggaccgct 300 ngcgcgtgcc ctggatgtca ccactttngc ccggacaact gacggtnana caaggatggg 360 gggtgganan nccngtaanc caagaanggg naggac 396 <210> SEQ ID NO 89 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 37, 76, 230, 295, 306, 333, 346, 370, 376, 377, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 89 gagagaacag taaacatcca gccttagcat ctctcangag tactgcagat cttcattagc 60 tatattcaca tggagnaatg ctattcaacc tatttctctt atcaaaacta attttgtatt 120 ctttgaccaa tgttcctaaa ttcactctgc ttctctatct caatcttttt cccctttctc 180 atctttcctc cttttttcag tttctaactt tcactggttc tttggaatgn tttttctttc 240 atctcttttc ttttacattt tggggtgtcc cctctctttt cttaccctct ttctncatcc 300 ttcttnttct tttgaattgg ctgcccttta tcntctcatc tgctgncatc ttcatttctc 360 ctccctcctn tttccnntca ttctactctc tcccnt 396 <210> SEQ ID NO 90 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 82, 110, 115, 120, 121, 125, 126, 129, 131, 140, 141, 144, 145, 146, 148, 149, 150, 153, 154, 157, 158, 160, 161, 163, 164, 166, 170, 172, 173, 174, 175, 179, 182, 184, 189, 193, 194, 195, 200, 206, 213, 215, 217, 218, 219, 220, 227 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 228, 231, 233, 236, 241, 247, 248, 249, 250, 254, 259, 262, 269, 273, 274, 275, 280, 281, 282, 286, 287, 289, 293, 294, 301, 302, 304, 309, 311, 318, 319, 324, 325, 330, 331, 333, 334, 336, 337, 341, 342, 343, 344, 349, 352, 353, 358 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 361, 365, 367, 373, 377, 381, 385, 386, 387, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 90 gggcgccggc gcgccccccc acccccgccc cacgtctcgt cgcgcgcgcg tccgctgggg 60 gcggggagcg gtcgggccgg cngcggtcgg ccggcggcag ggtggtgcgn tttcnttttn 120 nattnnccnc nttcttcttn nttnnncnnn ctnntanncn ntnncnttcn cnnnntttnc 180 tntntcttna ccnnnttttn taatcntctt ctncntnnnn tctcttnnat ntnttnctta 240 nttcctnnnn tttnttctnt cntttctcnc ctnnntctcn nnctcnncnc tcnncatttt 300 nntnttttnt nccttctnnt cttnnttctn ntnntnnttt nnnnttctnt tnntcatntt 360 ncctntntta ctntcanctt ntatnnncct cntttt 396 <210> SEQ ID NO 91 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1, 3, 8, 9, 16, 17, 18, 21, 22, 32, 33, 45, 50, 63, 64, 68,75, 82, 92, 95, 98, 102, 106, 108, 110, 111, 116, 121, 135, 151, 154, 158, 162, 167, 170, 176, 181, 185, 187, 209, 212, 215, 225, 231, 245, 257, 278, 283, 288, 290, 292, 293 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 312, 324, 326, 330, 331, 333, 334, 344, 345, 349, 351, 352, 357, 358, 382, 384, 390, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 91 ntntcctnna tttttnnntc nncttttttt tnnaattttt ctttnttttn tttataaaaa 60 tcnncacnta aaacngcgga anaggggatt tnttnttngg gngtancncn nggccncaaa 120 naaccccaaa aatancccaa aatgcacagg nccngggnaa angaccnacn tgggtntttt 180 ntttntnaac aaggggggtt ttaaagggna tnggnatcaa agggnataaa ntttaaacct 240 ttganaaatt ttttaanagg cttgcccccc actttggncc ccnccccncn gnngggatcc 300 aatttttttt cnttggggct cccngncccn nannttccgg gttnntggnc nntcctnntt 360 tttttttttt tgccttcacc cntnccattn cntttt 396 <210> SEQ ID NO 92 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 3, 7, 8, 9, 11, 31, 149, 152, 221, 233, 259, 263, 264, 265, 266, 274, 278, 279, 283, 286, 294, 302, 307, 309, 310, 311, 314, 316, 320, 343, 351, 363, 372, 377, 386, 393 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 92 ctntttnnnt ntttttttcc ccatcatcca naaatgggtt ttattctcag ccgagggaca 60 gcaggactgg taaaaactgt caggccacac ggttgcctgc acagcacccc catgcttggt 120 agggggtggg agggatggcg ggggctggnt gnccacaggc cgggcatgac aaggaggctc 180 actggaggtg gcacactttg gagtgggatg tcgggggaca ncttctttgg tanttgggcc 240 acaagattcc caaggatanc acnnnnactg attnccannc tanagncaag cggntggcca 300 tntgtangnn nttntntatn tgactattta tagattttta tanaacaggg naagggcata 360 ccncaaaagg gnccaanttt ttaccnccgg gcnccc 396 <210> SEQ ID NO 93 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 290, 304, 313, 320, 325, 333, 337, 348, 351 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 93 gctgccacag atctgttcct ttgtccgttt ttgggatcca caggccctat gtatttgaag 60 ggaaatgtgt atggctcaga tcctttttga aacatatcat acaggttgca gtcctgaccc 120 aagaacagtt ttaatggacc actatgagcc cagttacata aagaaaaagg agtgctaccc 180 atgttctcat ccttcagaag aatcctgcga acggagcttc agtaatatat cgtggcttca 240 catgtgagga agctacttaa cactagttac tctcacaatg aaggacctgn aatgaaaaat 300 ctgnttctaa ccnagtcctn tttanatttt agngcanatc cagaccancg ncggtgctcg 360 agtaattctt tcatgggacc tttggaaaac tttcag 396 <210> SEQ ID NO 94 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 115, 204, 205, 243, 266, 276, 316, 319, 355, 357, 364 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 94 tgccttaacc agtctctcaa gtgatgagac agtgaagtaa aattgagtgc actaaacgaa 60 taagattctg aggaagtctt atcttctgca gtgagtatgg cccaatgctt tctgnggcta 120 aacagatgta atgggaagaa ataaaagcct acgtgttggt aaatccaaca gcaagggaga 180 tttttgaatc ataataactc atanngtgct atctgtcagt gatgccctca gagctcttgc 240 tgntagctgg cagctgacgc ttctangata gttagnttgg aaatggtctt cataataact 300 acacaaggaa agtcanccnc cgggcttatg aggaattgga cttaataaat ttagngngct 360 tccnacctaa aatatatctt ttggaagtaa aattta 396 <210> SEQ ID NO 95 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 11, 16, 31, 36, 42, 49, 53, 56, 57, 60, 67, 70, 84, 89, 91, 92, 99, 105, 106, 112, 120, 121, 125, 127, 128, 133, 137, 141, 151, 152, 153, 154, 155, 162, 166, 167, 168, 174, 177, 179, 186, 188, 194, 195, 199, 203, 205, 213, 217, 221 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 227, 232, 235, 236, 240, 242, 260, 261, 265, 266, 291, 297, 318, 325, 330, 339, 348, 351, 352, 354, 356, 362, 364, 372, 380, 392, 395, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 95 cctcccaccc ncttanttca tgagattcga naatgncact tntgtgctnt ttnctnnttn 60 tattctnacn atttctttct tggngcggna nnaatcccnt ttttnngggc gnctctcccn 120 ncttntnntt tcntggngct ntcccttttc nnnnnaaact tntacnnngt ttanaantnt 180 ttctgnangg gggnntccna aananttttt ccncctncct nattccnctc tnaannctcn 240 cnaattgttt cccccccccn ntagnntatt ttttctaaaa aattaactcc nacgganaaa 300 attttcccta aaatttcncc tccanatttn gaaaaaacnc gcccgganct nntntncgaa 360 tntnaatttt tnaaaaaaan ttattttcat cnggnn 396 <210> SEQ ID NO 96 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 161, 193, 253, 259, 281, 288, 299, 309, 318, 319, 335, 340, 344, 352, 355, 356, 387, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 96 cctgggtacc aaatttcttt atttgaagga atggtacaaa tcaaagaact taagtggatg 60 ttttggacaa cttatagaaa aggtaaagga aaccccaaca tgcatgcact gccttggcga 120 ccagggaagt caccccacgg ctatggggaa attagcccga ngcttaactt tcattatcac 180 tgcttccaag ggngtgcttg gcaaaaaaat attccgccaa ccaaatcggg cgctccatct 240 tgcccagttg gtnccgggnc cccaattctt ggatgctttc ncctcttntt ccggaatgng 300 ctcatgaant cccccaanng gggcattttg ccagnggccn tttngccatt cnagnnggcc 360 tgatccattt tttccaatgt aatgccnctt cattgn 396 <210> SEQ ID NO 97 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 13, 15, 16, 19, 23, 31, 38, 39, 41, 45, 68, 94, 95, 100, 119, 131, 133, 141, 144, 164, 171, 182, 186, 190, 191, 195, 196, 198, 213, 229, 231, 235, 239, 247, 257, 265, 269, 272, 278, 279, 286, 289, 291, 306, 309, 310, 312, 317, 320 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 321, 327, 328, 337, 340, 343, 351, 360, 361, 368, 375, 381, 385, 386, 387, 388 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 97 ctcaccctcc tcntnnttnt canaatattg ngaacttnnt nctgntcgaa tcactggcat 60 taaagganca ctagctaatg gcactaaatt tacnnactan ggaaactttt ttataatant 120 gcaaaaacat ntnaaaaaga ntgnagttcg cccatttctg cttnggaaga nctcttcact 180 tntaancccn natgnngncc tttgggtcaa aanctccgcg attattacng ngttncccnc 240 tatttgncct tcctttntcc ccaangccnc anatttcnna actttnccnt naaatgcctt 300 tatttnatnn cntttcnacn ncttaanntt ccctttnaan aangatccct ncttcaaatn 360 ntttcccngt tcctngcatt ncccnnnnat ttctct 396 <210> SEQ ID NO 98 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 130, 202, 285, 296, 299, 308, 314, 321, 322, 336, 373 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 98 acagggacaa tgaagccttt gaagtgccag tctatgaaga ggccgtggtg ggactagaat 60 cccagtgccg cccccaagag ttggaccaac caccccctac agcactgttg tgataccccc 120 agcacctgan gaggaacaac ctaccatcca gaggggccag gaaaagccaa actggaacag 180 aggcgaatgg ctcagagggg tncatggcca agaaggaagc cctggaagaa cttcaatcac 240 cttcggtttc gggaccaccg gcttgtgtcc ctgttctgac tgcanaactt ggcgcngtnc 300 cccattanaa cctntgactc nncccttgct ataagnctgt tttggcccct gatgatgata 360 gggtttttat gangacactt gggcaccccc ttaatg 396 <210> SEQ ID NO 99 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1, 4, 13, 15, 26, 31, 43, 46, 48, 52, 54, 55, 60, 62, 68, 72, 93, 112, 118, 119, 122, 131, 132, 133, 134, 145, 147, 152, 157, 163, 164, 186, 190, 225, 231, 239, 246, 247, 250, 255, 262, 285, 314, 316, 319, 325, 332, 339, 343, 345 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 348, 351, 352, 355, 357, 361, 370, 387 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 99 nttntttttc cgncnaaagg gcaagngttt ncatctttcc tgnccncnca ananngggtn 60 tntgtgcntt tnttttttcc caaaacccgg gtnggggaca ccttttgagg anccactnnt 120 cntccggggc nnnnttttag aaggngncta anaagcntct tgnnggggga aaaacatctt 180 tttgcncccn acataccccc aagggggggg ggtgtctggg agganactaa ngacttttnt 240 tttttnnccn caaanaactg anggccccca ttgctccccc cccantcttt aaaaaacccc 300 ttcaatttcc ttgncnggna aaaanggttg gnaaaaaang agngngcntc nnttncnttt 360 natggaaggn aaaaggtttt tggttgnaaa accccg 396 <210> SEQ ID NO 100 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 229, 286, 303, 312, 334, 335, 348, 350, 357, 364, 371, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 100 ctaacacggt gaaaccctgt ctctactaaa aatacaaaaa aattagccag gcgtggtggc 60 gggcacctgt agtcccagct gctcaggaag ctgaggcagg agaatggcgt gaacccagaa 120 ggcggagctt gcagtgagct gagatcgtgt cagtgcactc cagcctgggc gacagagcga 180 gactcccgct caaaaaaaaa aaaaaaaaga gaaaagaaaa agctgcagng agctgggaat 240 gggccctatc ccctccttgg ggatcaatga gacccctttt caaaanaaaa aaaaaaataa 300 tgngattttg gnaacatatg gcactggtgc ttcnnggaat tctgtttntn ggcatgnccc 360 cctntgactg nggaaaaatc cagcaggagg cccana 396 <210> SEQ ID NO 101 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 93, 99, 100, 111, 168, 172, 174, 199, 209, 216, 218, 219, 227, 242, 243, 269, 272, 297, 300, 301, 308, 315, 317, 323, 331, 341, 344, 348, 357, 359, 363, 364, 366, 376, 379, 386, 389, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 101 agttataact caacagttca tttatatgct gttcatttaa cagttcattt aaacagttca 60 ttataactgt ttaaaaatat atatgcttat agncaaaann tgttgtggcg nagttgttgc 120 cgcttatagc tgagcattat ttcttaaatt cttgaatgtt cttttggngg gntnctaaaa 180 ccgtatatga tccattttna tgggaaacng aattcntnnc attatcncac cttggaaata 240 cnnaacgtgg gggaaaaaaa tcattcccnc cntccaaaac tatacttctt ttatctngan 300 nttcttgntc ctgcncnggt ttngaatata nctgggcaaa nggntttncc aaatccntnt 360 acnntncttt gggaantanc ggcaantcnt cncttt 396 <210> SEQ ID NO 102 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 17, 93, 136, 183, 317 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 102 actatacata agaacangct cacatgggag gctggaggtg ggtacccagc tgctgtggaa 60 cgggtatgga caggtcataa acctagagtc agngtcctgt tggcctagcc catttcagca 120 ccctgccact tggagnggac ccctctactc ttcttagcgc ctaccctcat acctatctcc 180 ctnctcccat ctcctacgga ctggcgccaa atggctttcc tgccaatttt gggatcttct 240 ctggctctcc agcctgctta ctcctctatt tttaaagggc caaacaaatc ccttctcttt 300 ctcaaacaca gtaatgnggc actgacccta ccacacctca tgaagggggc ttgttgcttt 360 tatttgggcc cgatctgggg ggggcaaaat attttg 396 <210> SEQ ID NO 103 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 91, 174, 176, 188, 201, 214, 254, 277, 299, 325, 349, 355, 365, 372, 390 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 103 ttgtgttggg actgctgata ggaagatgtc ttcaggaaat gctaaaattg ggcaccctgc 60 cccaacttca aagccacagc tggtatgcca natggtcagg ttaaagatat caacctgctg 120 actacaaagg aaaatatggt ggggtcttct tttaccctct tgacttccct ttgngngccc 180 cccgaganca ttgctttccg ngatagggca aaanaaatta aaaaacttaa ctggccagtg 240 aatggggctt ctgnggatct ccttctggca ttacatnggc aatccctaaa aaacaagang 300 actgggaccc ataacattct tttgnatcaa ccgaagcccc cattgttang atatngggct 360 taaangctga tnaagcatct cgtccgggcn ttttat 396 <210> SEQ ID NO 104 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 32, 53, 86, 141, 154, 156, 181, 182, 197, 204, 219, 224, 226, 229, 232, 245, 253, 260, 262, 271, 273, 276, 292, 301, 303, 305, 321, 325, 332, 343, 352, 382, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 104 aagggagggc gcgccaagac cttcccactc gngcacactg ggggcgccga cangacgcaa 60 cccagtccaa cttggatacc cttggnttta gttctcggac acttctttta tctctccgtc 120 gcaacttgtc aagttctcaa nactgtctct ctgngntatc ttttttcttc gctgctcttc 180 nncccccgac gtatttntca aaangtctgc aattgttgna tacntnganc tncaccactg 240 ttacnaggtc atnaatttcn cntcaactct ntnccncttg ttccctgata tntcggccgg 300 ngncnccaat tctgtatttt nctcntcaac gntctcactt ttncctcctc cnggccactt 360 tctccccttc cttattccgg cnttgtttgc cnccat 396 <210> SEQ ID NO 105 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 57, 306, 356, 388, 391 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 105 tcaatagcca gccagtgttc atttttatcc ttgagctttt agtaaaaact tcctggnttt 60 atttttagtc attgggtcat acagcactaa agtctgctat ttatggaaac taactttttt 120 gtttttaatc caggccaaca tgtatgtaaa ttaaattttt agataattga ttatctcttt 180 gtactacttg agatttgatt atgagatgtg catattgctt tgggaagagc tcgaggaagg 240 aaataattct ctcctttggt ttgaacctca actagataaa ccctaggaat tgttaactgc 300 acaagnattt tcattccaca aaacctgagg cagctctttt gccagagcgt tcctgnaccc 360 ccccacccca cttgccttgg gtctttanaa ngagcc 396 <210> SEQ ID NO 106 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 106 gctgtgtagc acactgagtg acgcaatcaa tgtttactcg aacagaatgc atttcttcac 60 tccgaagcca aatgacaaat aaagtccaaa ggcattttct cctgtgctga ccaaccaaat 120 aatatgtata gacacacaca catatgcaca cacacacaca cacacccaca gagagagagc 180 tgcaagagca tggaattcat gtgtttaaag ataatccttt ccatgtgaag tttaaaatta 240 ctatatattt gctgatggct agattgagag aataaaagac agtaaccttt ctcttcaaag 300 ataaaatgaa aagcaattgc tcttttcttc ctaaaaaatg caaaagattt acattgctgc 360 caaatcattt caactgaaaa gaacagtatt gctttg 396 <210> SEQ ID NO 107 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 12, 210, 257, 261, 271, 302, 311, 314, 318, 368, 374, 385, 389, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 107 ttcacagaac anggtggttt attatttcaa tagcaaagag ctgaaaaatg tcgggtccca 60 taaaggagca gaacctgacc cagagcctgc agtacatttc caccccacag gggtgcaggc 120 tgggccaggc agggccaaag gcagcagaaa tgggagtaag agactgtgcc cactgagaag 180 ctctgctggg tgtgggcagg tgggcatgan atgatgatga tgtagtgtaa ggaccaggta 240 ggcaaaacct gtcaggnttg ntgaatgtca nagtggatcc aaaaggctga gggggtcgtc 300 anaaggccgg nggncccncc cttgcccgta tgggccttca aaaagtatgc ttgctcatcc 360 gttgtttncc ccanggagct gccanggana aggctn 396 <210> SEQ ID NO 108 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 280, 281, 286, 305, 311, 313, 323, 326, 327, 340, 352, 356, 363, 369, 378, 388, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 108 gcctgctttt gatgatgtct acagaaaatg ctggctgagc tgaacacatt tgcccaattc 60 caggtgtgca cagaaaaccg agaatattca aaattccaaa tttttttctt aggagcaaga 120 agaaaatgtg gccctaaagg gggttagttg aggggtaggg ggtagtgagg atcttgattt 180 ggatctcttt ttatttaaat gtgaatttca acttttgaca atcaaagaaa agacttttgt 240 tgaaatagct ttactgcttc tcacgtgttt tggagaaaan natcanccct gcaatcactt 300 tttgnaactg ncnttgattt tcngcnncca agctatatcn aatatcgtct gngtanaaaa 360 tgncctggnc ttttgaanga atacatgngt gntgct 396 <210> SEQ ID NO 109 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 237, 279, 284, 291, 305, 307, 308, 313, 326, 343, 351, 366, 376, 392, 394, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 109 ggccgtaggc agccatggcg cccagcccgg aatggcatgg tcttgaagcc ccacttccac 60 aaggactggc agcggcgcgt ggccacgtgg ttcaaccagc cggcccggaa gatccgcaga 120 cgtaaggccc ggcaagccaa ggcgcgccgc atcgctccgc gccccgcgtc gggtcccatc 180 cggcccatcg tgcgctgccc acggttcggt accacacgaa gggcgcgccg gcgcggnttc 240 agcctggagg agctcagggt ggccggattt acaagaagng gccngacatc ngtattcttg 300 ggatncnnga agnggaacaa gtcacngagt ccttgcagcc acntcagcgg ntgatgacac 360 cgttcnaact catctnttcc caagaaacct cngnnc 396 <210> SEQ ID NO 110 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1, 2, 12, 13, 16, 18, 29, 39, 60, 66, 70, 86, 90, 104, 121, 122, 127, 128, 146, 165, 171, 172, 173, 176, 188, 189, 193, 195, 205, 210, 211, 224, 226, 227, 231, 233, 240, 243, 244, 248, 249, 255, 257, 258, 260, 266, 268, 272, 273, 275 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 278, 280, 287, 292, 294, 303, 308, 312, 315, 320, 322, 332, 333, 334, 335, 345, 347, 351, 363, 364, 369, 371, 372, 379, 381, 382, 386, 391, 393 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 110 nntgggctcc tnncantnat aataaaccng actcatacnc cacaaggaga tgaacaggan 60 tatgtncatn ctgacgcgga aacagngcan ggagctgagg aggngccaag atgagaccta 120 nnggccnngg tgggcgcatt cccggnggag ggggccacta aggantacga nnntcnagcg 180 gctcttgnng gcngncctcc tcacncctgn ntattcgatt gtcncnnatg ncntcctatn 240 atnntcanna ttctntnntn atctcntnta cnncntcncn ttcatgntta cngntccctc 300 tcnttctnac cnttntctgn anctcctttc tnnnnctttc atctntnttc ngctttcttt 360 ctnnaatcnt nntttaacnt nntctncttt ntnatt 396 <210> SEQ ID NO 111 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 4, 7, 11, 16, 19, 25, 26, 30, 33, 39, 54, 60, 69, 75, 81, 99, 102, 130, 132, 143, 154, 156, 166, 180, 182, 188, 190, 192, 194, 198, 201, 226, 242, 253, 261, 264, 295, 305, 313, 315, 320, 323, 325, 330, 334, 337, 340, 344, 348, 349 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 351, 352, 357, 358, 359, 361, 362, 381, 387, 388, 389, 394 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 111 taangancat nctggnttnt gcctnnccgn ctnattgant gttaaaggca attntgtggn 60 tgtcccagng aatgncggct nattttcttt ccacattgng cncattcact cctcccactc 120 ttggcatgtn gngacataag canggtacat aatngnaaaa atctgnattt ctgatgccan 180 angggtanan cntnttgnat ntcattccat tgatatacag ccactntttt atttttgatc 240 ancggccttc ggntcactgc ncanggtact tgacctcagt gtcactatta tgggntttgg 300 tttcnctctt ttncnggccn ttntntttcn cacnttncan cttncttnnt nnaaaannna 360 nncactctct cttgctctct ngatacnnng tctnaa 396 <210> SEQ ID NO 112 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 172, 186, 378, 380, 382, 388 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 112 tcaacgtcac caattactgc catttagccc acgagctgcg tctcagctgc atggagagga 60 aaaaggtcca gattcgaagc atggatccct ccgccttggc aagcgaccga tttaacctca 120 tactggcaga taccaacagt gaccggctct tcacagtgaa cgatgttaaa gntggaggct 180 ccaagnatgg tatcatcaac ctgcaaagtc tgaagacccc tacgctcaag gtgttcatgc 240 acgaaaacct ctacttcacc aaccggaagg tgaattcggg gggctgggcc tcgctgaatc 300 acttggattc cacattctgc tatgcctcat gggactcgca gaacttcagg ctggccaccc 360 tgctcccacc atcactgntn gncaatantc acccag 396 <210> SEQ ID NO 113 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1, 2, 3, 4, 7, 8, 9, 10, 11, 65, 273, 279, 280, 289, 321, 338, 380 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 113 nnnnttnnnn nggagcctta atttcagagt tttattgtat tgcactaaag gaacagcagg 60 atggntatac aattttctct cattcagttt tgaaaatctg tagtacctgc aaattcttaa 120 gaataccttt accaccagat tagaacagta agcataataa ccaatttctt aataagtaat 180 gtcttacaaa taaaaacaca tttaaaatag ctttaaatgc attcttcaca agtaattcag 240 catatatttt atatcatggt tacttatgct tangaattnn agcaggatnt ttattctttt 300 gatggaaata tgggaaaact ntattcatgc atatacangg ataatattca gcgaagggaa 360 aatcccgttt ttattttggn aatgattcat atataa 396 <210> SEQ ID NO 114 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 40, 82, 114, 116, 146, 164, 166, 174, 185, 212, 215, 219, 224, 236, 242, 254, 258, 263, 270, 286, 299, 308, 327, 328, 329, 345, 363, 378, 382, 385 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 114 aaatgggaca acgtgattct tttgttttaa ataaatactn agaacacgga cttggctcct 60 acaagcattt ggactctaag gnttagaact ggagagtctt acccatgggc cccncncagg 120 gacgccacgg ttccctccca ccccgngatc aagacacgga atcngntggc gatngttgga 180 tcgcnatgtg ccccttatct atagccttcc cnggncatnt acangcagga tgcggntggg 240 anaactacaa ctgnaatntc tcnaacggtn atggtcccca ccgatnaaga ttctacctng 300 tcttttcntc ccctggagtg tgagtgnnng aggaagaagc ccttncctta catcaccttt 360 tgnacttctg aacaaganca anacnatggc cccccc 396 <210> SEQ ID NO 115 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 277, 297, 321, 341, 381, 391 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 115 ccgcctggtt cggcccgcct gcctccactc ctgcctctac catgtccatc agggtgaccc 60 agaagtccta caaggtgtcc acctctggcc cccgggcctt cagcagccgc tcctacacga 120 gtgggcccgg ttcccgcatc agctcctcga gcttctcccg agtgggcagc agcaactttc 180 gcggtggcct ggcggcggct atggtggggc cagcggcatg ggaggcatca cccgcagtta 240 cggcaaccag agcctgctga gccccttgcc tggaggngga ccccaacatc aagccgngcg 300 cacccaggaa aaggagcaga ncaagaccct caacaacaag nttgcttctt catagacaag 360 ggaccggtcc ttgaacagca naacaagatg ntggag 396 <210> SEQ ID NO 116 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 267, 290, 343, 351, 376 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 116 atctcagttt actagctaag tgactttggg caagggattt aacctctcgt ccctcagttt 60 cctcctatgt aaaatgacaa ggataatagt accaacccaa tgtagattaa atgagtttac 120 gaagtgttag aatagtgctt ggcacattag tgctttacaa ctgctatttt gattgttgtt 180 gtgggctctc tcaaatgcat tgtctctaga tgccagtgac ccaggtcaaa atttaccttt 240 aaccaagctg catgtttccc agactgntgc acagtcctct accctgagan aaagcttcca 300 cccaaggata cttttacttt ctgctggaaa actgatgagc aanggcaaca ngggacactt 360 atcgccaact ggaaangaga aattcttcct tttgct 396 <210> SEQ ID NO 117 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 228, 267, 318, 331, 357, 368, 376 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 117 aaacattttt taataaaatt cctatagaaa gctcagtcat agggcaaata ctcagttctc 60 tttcccatat caccgaggat tgagagctcc caatattctt tggagaataa gcagtagttt 120 tgctggatgt tgccaggact cagagagatc acccatttac acattcaaac cagtagttcc 180 tattgcacat attaacatta cttgccccta gcaccctaaa tatatggnac ctcaacaaat 240 aacttaaaga tttccgtggg gcgcganacc atttcaattt gaactaatat ccttgaaaaa 300 aatcacatta ttacaagntt taataaatac nggaagaaga gctggcattt ttctaanatc 360 tgaattcnga cttggnttta ttccataaat acggtt 396 <210> SEQ ID NO 118 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 4, 5, 12, 14, 15, 16, 24, 59, 80, 87, 225, 280, 286, 287, 295, 297, 298, 337, 349, 362, 375, 387, 394 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 118 accnncacct gntnnntttt aacnattaca acttctttat atggcagttt ttactgggng 60 cctaacactc tctttactgn ctcaagngga agtccaaaca aatttcattt ttgtagtaaa 120 aaatctttat ttccaaaatg atttgttagc caaaagaact ataaaccacc taacaagact 180 ttggaagaaa gagacttgat gcttcttata aattccccat tgcanacaaa aaataacaat 240 ccaacaagag catggtaccc attcttacca ttaacctggn tttaannctc caaancnnga 300 tttaaaaatg accccactgg gcccaatcca acatganacc taggggggnt tgccttgatt 360 angaatcccc cttanggact ttatctnggc tganaa 396 <210> SEQ ID NO 119 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 251, 281, 298, 301, 308, 326, 332, 337, 351, 358, 362, 388, 394 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 119 atggccagct cactttaaat accacctcaa gactcatcga aatgaccgct ccttcatctg 60 tcctgcagaa ggttgtggga aaagcttcta tgtgctgcag aggctgaagg tgcacatgag 120 gacccacaat ggagagaagc cctttatgtg ccatgagtct ggctgtggta agcagtttac 180 tacagctgga aacctgaaga accaccggcg catccacaca ggagagaaac ctttcctttg 240 tgaagcccaa ngatgtggcc gtcctttgct gagtattcta ncttcgaaaa catctggngg 300 ntactcanga gagaaagcct cattantgcc antctgnggg aaaaccttct ntcagagngg 360 angcaggaat gtgcatatta aaaagctncc ttgnac 396 <210> SEQ ID NO 120 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 261, 263, 265, 272, 273, 288, 308, 310, 330, 379 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 120 catgggtcag tcggtcctga gagttcgaag agggcacatt cccaaagaca ttcccagtca 60 tgaaatgtag aagactggaa aattaagaca ttatgtaaag gtagatatgg cttttagagt 120 tacattatgc ttggcatgaa taaggtgcca ggaaaacagt ttaaaattat acatcagcat 180 acagactgct gttagaaggt atgggatcat attaagataa tctgcagctc tactacgcat 240 ttattgttaa ttgagttaca nangncattc annactgagt ttatagancc atattgctct 300 atctctgngn agaacatttg attccattgn gaagaatgca gtttaaaata tctgaatgcc 360 atctagatgt attgtaccna aaggggaaaa ataaca 396 <210> SEQ ID NO 121 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 77, 125, 130, 142, 155, 162, 166, 176, 204, 227, 242, 243, 245, 246, 249, 251, 252, 265, 279, 306, 310, 314, 336, 341, 354, 367, 382, 385, 390, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 121 tttttttttt ttttttttaa aatcaagtta tgtttaataa acattaataa atgtttactt 60 aaaagggtta ataaacnttt actacatggc aaattatttt agctagaatg cttttggctt 120 caagncatan aaaccagatt cnaatgccct taaanaattt tnaaanatcc attgangggg 180 ataactgtaa tccccaaggg gaanagggtt gggtatgaca ggtacanggg gccagcccag 240 tnntnncana nncagactct taccntcttt ctgctgtgnc accctcaggc attggctcca 300 ttctcngggn tgcncatggg aagatggctt tggacntaac nacacccttt tgtncacgta 360 aaggccngat gcagggtcaa anagnttccn ccatnt 396 <210> SEQ ID NO 122 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 122 gtcgacatgg ctgccctctg ggctcccaga acccacaaca tgaaagaaat ggtgctaccc 60 agctcaagcc tgggcctttg aatccggaca caaaaccctc tagcttggaa atgaatatgc 120 tgcactttac aaccactgca ctacctgact caggaatcgg ctctggaagg tgaagctaga 180 ggaaccagac ctcatcagcc caacatcaaa gacaccatcg gaacagcagc gcccgcagca 240 cccaccccgc accggcgact ccatcttcat ggccaccccc tgcggtggac ggttgaccac 300 cagccaccac atcatcccag agctgagctc ctccagcggg atgacgccgt ccccaccacc 360 tccctcttct tctttttcat ccttctgtct ctttgt 396 <210> SEQ ID NO 123 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 74, 94, 142, 149, 194, 219, 233, 279, 316, 335, 368 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 123 gccctttttt tttttttttt tttcctagtg ccaggtttat tccctcacat gggtggttca 60 catacacagc acanaggcac gggcaccatg gganagggca gcactcctgc cttctgaggg 120 gatcttggcc tcacggtgta anaagggana ggatggtttc tcttctgccc tcactagggc 180 ctagggaacc cagnagcaaa tcccaccacg ccttccatnt ctcagccaag ganaagccac 240 cttggtgacg tttagttcca accattatag taagtggana agggattggc ctggtcccaa 300 ccattacagg gtgaanatat aaacagtaaa ggaanataca gtttggatga ggccacagga 360 aggagcanat gacaccatca aaagcatatg caggga 396 <210> SEQ ID NO 124 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 124 gaccattgcc ccagacctgg aagatataac attcagttcc caccatctga ttaaaacaac 60 ttcctccctt acagagcata caacagaggg ggcacccggg gaggagagca catactgtgt 120 tccaatttca cgcttttaat tctcatttgt tctcacacca acagtgtgaa gtgcgtggta 180 taatctccat ttcaaaacca aggaagcagc ctcagagtgg tcgagtgaca cacctcacgc 240 aggctgagtc cagagcttgt gctcctcttg attcctggtt tgactcagtt ccaggcctga 300 tcttgcctgt ctggctcagg gtcaaagaca gaatggtgga gtgtagcctc cacctgatat 360 tcaggctact cattcagtcc caaatatgta ttttcc 396 <210> SEQ ID NO 125 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 43, 88, 91, 94, 139, 141, 150, 163, 193, 202, 212, 215, 222, 238, 253, 256, 286, 297, 331, 343, 350, 360, 376, 385, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 125 cccttttttt tttttttttt tttttttttt ttttttactt tgnaacaaaa atttattagg 60 attaagtcaa attaaaaaac ttcatgcncc nccncttgtc atatttacct gaaatgacaa 120 agttatactt agcttgagng naaaacttgn gccccaaaaa ttntgtttgg aaagcaaaaa 180 aataattgat gcncatagca gngggcctga tnccnccaca gngaatgttg tttaaggnct 240 aacaaacagg ggncancaaa gcatacatta cttttaagct ttgggnccaa ggaaaangtc 300 attccctacc tccttcaaaa gcaaactcat natagcctgg gcncctaggn ctggagcctn 360 ttttttcgag tctaanatga acatntggat ttcaan 396 <210> SEQ ID NO 126 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 126 cgcgtcgact cgcaagtgga atgtgacgtc cctggagacc ctgaaggctt tgcttgaagt 60 caacaaaggg cacgaaatga gtcctcaggt ggccaccctg atcgaccgct ttgtgaaggg 120 aaggggccag ctagacaaag acaccctaga caccctgacc gccttctacc ctgggtacct 180 gtgctccctc agccccgagg agctgagctc cgtgcccccc agcagcatct gggcggtcag 240 gccccacgac ctggacacgc tggggctacg gctacagggc ggcatcccca acggctacct 300 ggtcctagac ctcagcatgc aagaggccct ctcggggacg ccctgcctcc taggacctgg 360 acctgttctc accgtcctgg cactgctcct agcctc 396 <210> SEQ ID NO 127 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 15 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 127 tttttttttt ttggnggtaa aatgcaaatg ttttaaaata tgtttatttt gtatgtttta 60 caatgaatac ttcagcaaag aaaataatta taatttcaaa atgcaatccc tggatttgat 120 aaatatcctt tataatcgat tacactaatc aatatctaga aatatacata gacaaagtta 180 gctaatgaat aaaataagta aaatgactac ataaactcaa tttcagggat gagggatcat 240 gcatgatcag ttaagtcact ctgccacttt ttaaaataat acgattcaca tttgcttcaa 300 tcacataaac attcattgca ggagttacac ggctaatcat tgaaaattat gatctttgtt 360 agcttaaaag aaaattcagt ttaatacaaa gacatt 396 <210> SEQ ID NO 128 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 220, 244, 351, 384 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 128 gccctttttt ttttttttta aaggcaaata aaataagttt attgggatgt aaccccatca 60 taaattgagg agcatccata caggcaagct ataaaatctg gaaaatttaa atcaaattaa 120 attctgcttt taaaaaggtg ccttaagtta accaagcatt ttgataacac attcaaattt 180 aatatataaa aatagatgta tcctggaaga tataatgaan aacatgccat gtgtataaat 240 tcanaatacg ctttttacac aaagaactac aaaaagttac aaagacagcc ttcaggaacc 300 acacttagga aaagtgagcc gagcagcctt cacgcaaagc ctccttcaaa naagtctcac 360 aaagactcca gaaccagccg agtntgtgaa aaagga 396 <210> SEQ ID NO 129 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 104, 164, 177, 204, 217, 234, 273, 312, 350, 353, 370 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 129 gccctttttt tttttttttt ttttactcag acaggcaata tttgctcaca tttattctct 60 tgcatcgtaa atagtagcca actcacaaaa ataaagtata caanaatgta atatttttta 120 aaataagatt aacagtgtaa gaaggaaaat ctcaaaaaaa gcanatagac aatgtanaaa 180 attgaaatga aatcccacag taanaaaaaa aaaacanaaa agtgcctatt taanaattat 240 gctacatgtg gaacttaact agaccatttt aanaaagacc aatttctaat gcaaattttc 300 tgaggttttc anattttatt tttaaaatat gttatagcta catgttgtcn acncggccgc 360 tcgagtctan agggcccgtt taaacccgct gatcag 396 <210> SEQ ID NO 130 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 23, 24, 26, 32, 56, 191, 286, 355 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 130 cgcccttttt tttttttttt tanngnacgt gnctttattt ctggatgata taaaanaaaa 60 aacttaaaaa acaccccaaa ccaaacacca atggatcccc aaagcgatgt gactccctct 120 tcccacccgg ataaatagag acttctgtat gtcagtctac cctcccgccc ccataacccc 180 ctctgctata nacatactct gggtatatat tactctactc ggcaatagac atctcccgaa 240 aatagaattc ctgccctgac acctgactct tccctggccg catcanacca cccgccactg 300 tagcacactg gtgtccttgc cccctgtggt cagggccatg ctgtcatccc acaanaaggc 360 cacatttgtc acatggctgc tgtgtccacc gtactt 396 <210> SEQ ID NO 131 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 49, 68, 69, 83, 88, 93, 136, 140, 154, 158, 166, 167, 168, 170, 172, 173, 187, 226, 239, 241, 247, 257, 259, 271, 293, 301, 318, 334, 336, 342, 344, 357, 377, 384 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 131 gccctttttt tttttttttt tttttttttt ttcagtttac acaaaaacnc tttaattgac 60 agtatacnnt tttccaaaat atnttttngt aanaaaatgc aataattatt aactatagtt 120 tttacaaaca agtttntcan taaattccag tgtncttnaa accccnnncn annaaaacat 180 atatganccc ccagttcctg ggcaaactgt tgaacattca ctgcanacaa aaagaccanc 240 nccaaanagt catctgngnc ctccatgctg ngtttgcacc aaacctgagg gancagctag 300 ngaccgtgac aaaagctntg ctacagtttt actntngccc tntntgcctc ccccatnatg 360 tttccttggt ccctcantcc tgtnggagta agttcc 396 <210> SEQ ID NO 132 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 69 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 132 cgcgtcgacc gcggccgtag cagccgggct ggtcctgctg cgagccggcg gcccggagtg 60 gggcggcgnt atgtaccttc cacattgagt attcagaaag aagtgatctg aactctgacc 120 attctttatg gatacattaa gtcaaatata agagtctgac tacttgacac actggctcgg 180 tgagttctgc tttttctttt taatataaat ttattatgtt ggtaaattta gcttttggct 240 tttcactttg ctctcatgat ataagaaaat gtaggttttc tctttcagtt tgaattttcc 300 tattcagtaa aacaacatgc tagaaaacaa acttttggaa aggcattgta actatttttt 360 caaatagaac cataataaca agtcttgtct taccct 396 <210> SEQ ID NO 133 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1, 17, 18, 20, 21, 25, 26, 30, 31, 40, 44, 45, 46, 51, 52, 66, 67, 68, 74, 89, 109, 122, 166, 193, 214, 218, 266, 269, 291, 307, 315, 348, 375, 378, 379, 386, 393 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 133 ntattacccc tcctggnnan ntggnnatan nctgcaaggn gatnnncccg nngaacttca 60 ctgatnnncc aatnaaaact gctttaaanc tgactgcaca tatgaattnt aatacttact 120 tngcgggagg ggtggggcag ggacagcaag ggggaggatt gggaanacaa tagacaggca 180 tgctggggat gcngcgggct ctatggcttc tgangcgnaa agaaccagct ggggctctag 240 ggggtatccc cacgcgccct gtagcngcnc attaaacgcg gcgggtgtgg nggttacttc 300 gcaaagngac cgatncactt gccagcgccc tagctgcccg ctcctttngc tttcttccct 360 tcctttctcg ccacnttnnc cggctntccc cgncaa 396 <210> SEQ ID NO 134 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 133, 144, 221, 229, 302, 358 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 134 tttttttttt ttctgctttt tatatgttta aaaatctctc attctattgc tgctttattt 60 aaagaaagat tactttcttc cctacaagat ctttattaat tgtaaaggga aaatgaataa 120 ctttacaatg ganacacctg gcanacacca tcttaaccaa agcttgaagt taacataacc 180 agtaatagaa ctgatcaata tcttgtgcct cctgatatgg ngtactaana aaaacacaac 240 atcatgccat gatagtcttg ccaaaagtgc ataacctaaa tctaatcata aggaaacatt 300 anacaaactc aaattgaagg acattctaca aagtgccctg tattaaggaa ttattcanag 360 taaaggagac ttaaaagaca tggcaacaat gcagta 396 <210> SEQ ID NO 135 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 135 gcgtcgacgc tggcagagcc acaccccaag tgcctgtgcc cagagggctt cagtcagctg 60 ctcactcctc cagggcactt ttaggaaagg gtttttagct agtgtttttc ctcgctttta 120 atgacctcag ccccgcctgc agtggctaga agccagcagg tgcccatgtg ctactgacaa 180 gtgcctcagc ttccccccgg cccgggtcag gccgtgggag ccgctattat ctgcgttctc 240 tgccaaagac tcgtgggggc catcacacct gccctgtgca gcggagccgg accaggctct 300 tgtgtcctca ctcaggtttg cttcccctgt gcccactgct gtatgatctg ggggccacca 360 ccctgtgccg gtggcctctg ggctgcctcc cgtggt 396 <210> SEQ ID NO 136 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 18, 185, 188, 191, 193, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 136 ttatgcttcc ggctcgtntg ttgtgtggaa ttgtgagcgg ataacaattt cacacaggaa 60 acagctatga ccatgattac gccaagctat ttaggtgaca ctatagaata ctcaagctat 120 gcatcaagct tggtaccgag ctcggatcca ctagtaacgg ccgccagtgt gctggaattc 180 gcggncgntc nantctagag ggcccgttta aacccgctga tcagcctcga ctgtgccttc 240 tagttgccag ccatctgttg tttgcccctc ccccgtgcct tccttgaccc tggaaggtgc 300 cactcccact gtcctttcct aataaaatga ggaaattgca tcgcattgtc tgagtaggtg 360 tcattctatt ctggggggtg gggtggggca ggacan 396 <210> SEQ ID NO 137 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 156, 216 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 137 tttttttttt ttctgctttg tacttgagtt tatttcacaa aaccacggag aaagatactg 60 aaatggagct ctttccagcc tccaagcaag gaggccccag cagccagtct ccagcccctt 120 gagccctttt tgttaggccc acacccaaaa gagganaacc agtgtgtgcg cgaaggtaca 180 tggcaaggca cttttgaaaa catcccagtt taccgnggtg aaattgaact tactctgaaa 240 cagatgaaaa gggacatgca aaattgctga gcacatggag gtgtttgtta gtaggtgaaa 300 atcatgtcct gggtataacc cagcttctcc aggttagggt gagccgccgt ctggatcagt 360 ggtggcgggc cacacaccag gatgagcgtg gacttc 396 <210> SEQ ID NO 138 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 69, 136, 265, 272 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 138 cccttttttt ttttttttac aaatgagaaa aatgtttatt aagaaaacaa tttagcagct 60 ctcctttana attttacaga ctaaagcaca acccgaaggc aattacagtt tcaatcatta 120 acacactact taaggngctt gcttactcta caactggaaa gttgctgaag tttgtgacat 180 gccactgtaa atgtaagtat tattaaaaat tacaaattgt ttggtgatta ttttgatgac 240 ctcttgagca gcagctcccc ccaanaatgc ancaatggta tgtggctcac cagctccata 300 tcggcaaaat tcgtggacat aatcatcttt caccattaca gataaaccat attcctgaag 360 gaagccagtg agacaagact tcaactttcc tatatc 396 <210> SEQ ID NO 139 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 51, 105, 126, 147, 210, 212, 236, 241, 258, 263, 348 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 139 ccgccctttt tttttttttt ttcacaaaag cactttttat ttgaggcaaa nagaagtctt 60 gctgaaagga ttccagttcc aagcagtcaa aactcaaccg ttagnggcac tattttgacc 120 tggtanattt tgcttctctt tggtcanaaa agggtattca ggttgtactt tccccagcag 180 ggtaaaaaga agggcaaagc aaactggaan anacttctac tctactgaca gggctnttga 240 natccaacat caagctanac acnccctcgc tggccactct acaggttgct gtcccactgc 300 tgagtgacac aggccatact acatttgcaa ggaaaaaaat gaggcaanaa acacaggtat 360 aggtcacttg gggacgagca ggcaaccaca gcttca 396 <210> SEQ ID NO 140 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 50, 60, 63, 100, 133, 135, 172, 183, 190, 196, 220, 240, 262, 266, 273, 278, 293, 327, 332, 341, 348, 355, 380, 391 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 140 tttttttttt tttttttttt tttttttctc atttaacttt tttaatgggn ctcaaaattn 60 tgngacaaat ttttggtcaa gttgtttcca ttaaaaagtn ctgattttaa aaactaataa 120 cttaaaactg ccncncccaa aaaaaaaaac caaaggggtc cacaaaacat tntcctttcc 180 ttntgaaggn tttacnatgc attgttatca ttaaccagtn ttttactact aaacttaaan 240 ggccaattga aacaaacagt tntganaccg ttnttccncc actgattaaa agnggggggg 300 caggtattag ggataatatt catttancct tntgagcttt ntgggcanac ttggngacct 360 tgccagctcc agcagccttn ttgtccactg ntttga 396 <210> SEQ ID NO 141 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 141 acgccgagcc acatcgctca gacaccatgg ggaaggtgaa ggtcggagtc aacggatttg 60 gtcgtattgg gcgcctggtc accagggctg cttttaactc tggtaaagtg gatattgttg 120 ccatcaatga ccccttcatt gacctcaact acatggttta catgttccaa tatgattcca 180 cccatggcaa attccatggc accgtcaagg ctgagaacgg gaagcttgtc atcaatggaa 240 atcccatcac catcttccag gagcgagatc cctccaaaat caagtggggc gatgctggcg 300 ctgagtacgt cgtggagtcc actggcgtct tcaccaccat ggagaaggct ggggctcatt 360 tgcagggggg agccaaaagg gtcatcatct ctgccc 396 <210> SEQ ID NO 142 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 142 acgcaggaga ggaagcccag cctgttctac cagagaactt gcccaggtca gaggtctgcg 60 tagaagccct tttctgagca tcctctcctc tcctcacacc tgccactgtc ctctgcgttg 120 ctgtcgaatt aaatcttgca tcaccatggt gcacttctgt ggcctactca ccctccaccg 180 ggagccagtg ccgctgaaga gtatctctgt gagcgtgaac atttacgagt ttgtggctgg 240 tgtgtctgca actttgaact acgagaatga ggagaaagtt cctttggagg ccttctttgt 300 gttccccatg gatgaagact ctgctgttta cagctttgag gccttggtgg atgggaagaa 360 aattgtagca gaattacaag acaagatgaa ggcccg 396 <210> SEQ ID NO 143 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 19, 48, 69, 122, 183, 227, 332, 390 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 143 tttttttttt tttccatana aaataggatt tattttcaca tttaaggnga acacaaatcc 60 atgttccana aatgttttat gcataacaca tcatgagtag attgaatttc tttaacacac 120 anaaaaatca aagcctacca ggaaatgctt ccctccggag cacaggagct tacaggccac 180 ttntgttagc aacacaggaa ttcacattgt ctaggcacag ctcaagngag gtttgttccc 240 aggttcaact gctcctaccc ccatgggccc tcctcaaaaa cgacagcagc aaaccaacag 300 gcttcacagt aaccaggagg aaagatctca gngggggaac cttcacaaaa gccctgagtt 360 gtgtttcaaa agccaagctc tggggtctgn ggcctg 396 <210> SEQ ID NO 144 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 221, 331 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 144 tttttttttt tttcgctctt tggtctgaca agaaaagagt tttaggtgtg tgaagtaggg 60 tgggaaaaaa ggtcagtttc aaattcagta acatatggta acactaagtt aggctgctgc 120 attcttttct ttgggtactt aagccagctg gcacttccac tttgtaacca attatattat 180 gatcaacaac taatcagtta gttcctcagc ttcaactgaa nagttcctga ttacctgatg 240 aaggacatac ttgctctggc ttcaattagc atgctgtcaa gcatccctct ccatgcttaa 300 catggcaaca caaaacccaa gagtccttct ntttttttca ttagccatga ataaacactc 360 acaaagggga agagtagaca ctgcttttag taaacg 396 <210> SEQ ID NO 145 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 45, 56, 61, 63, 120, 122, 147, 151, 158, 259, 262, 274, 339, 345, 353 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 145 tttttttttt tttttttcaa tggatccgtt agctttacta ctaanatctt gctganatca 60 nanaagggct tctgggcagg ctgagcactg ggggtgtgca acatggtaac tctgaataan 120 anaaaccctg agttttactg ggcaaanaaa naacaagngg taggtatgat ttctgaacct 180 ggaaatagcg aaaatgaagg aaattccaaa agcgcgtatt tccaaataat gacaggccag 240 caagaggaca ccaaacctnt anaaagaggt attntttctt ccagctactg atggctttgg 300 catcccacag gcacattcct ttggccttca ggatcttana tgcanatgtg ganagtcaag 360 aggtaggctg actctgagtc ttcagctaaa ttcttt 396 <210> SEQ ID NO 146 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 120, 130, 176, 180, 185, 208, 238, 254, 259, 261, 275, 285, 296, 347 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 146 tttttttttt ttttcattag caaggaagga tttatttttt cttttgaggg gagggcggaa 60 cagccgggat ttttggaaca ctacctttgt ctttcacttt gttgtttgtg tgttaacacn 120 aataaatcan aagcgacttt aaatctccct tcgcaggact gtcttcacgt atcagngcan 180 acaanaaaac agtggcttta caaaaaanat gttcaagtag gctgcacttt gcctctgngg 240 gtgaggcaca ctgngggana nacaaggtcc cctgnaacca gaggngggaa ggacanagct 300 ggctgactcc ctgctctccc gcattctctc ctccatgtgt tttgaanagg gaagcaacat 360 gttgaggtct gatcatttct acccagggaa cctgtt 396 <210> SEQ ID NO 147 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 147 acggggaagc caagtgaccg tagtctcatc agacatgagg gaatgggtgg ctccagagaa 60 agcagacatc attgtcagtg agcttctggg ctcatttgct gacaatgaat tgtcgcctga 120 gtgcctggat ggagcccagc acttcctaaa agatgatggt gtgagcatcc ccggggagta 180 cacttccttt ctggctccca tctcttcctc caagctgtac aatgaggtcc gagcctgtag 240 ggagaaggac cgtgaccctg aggcccagtt tgagatgcct tatgtggtac ggctgcacaa 300 cttccaccag ctctctgcac cccagccctg tttcaccttc agccatccca acagagatcc 360 tatgattgac aacaaccgct attgcacctt ggaatt 396 <210> SEQ ID NO 148 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 148 acgtcccatg attgttccag accatgactc ttcctggttg tgggtttgtt acagagcagg 60 agaagcagag gttatgacag ttatgcagac tttccccctc ctttttctct tttctcttcc 120 ccttgctttt ccactgtttc ttcctgctgc cacctgggcc ttgaattcct gggctgtgaa 180 gacatgtagc agctgcaggg tttaccacac gtgggagggc agcccagtac tgtccctctg 240 ccttccccac tttgagaata tggcagcccc tttcattcct ggcttggggt aggggagacc 300 attgaagtag aagcctcaaa gcagactttt ccctttactg tgtgtactcc aggacgaaga 360 aggaagatca tgcttgatac ttagattggt tttccc 396 <210> SEQ ID NO 149 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 214, 295 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 149 tttttttttt tttaaagagt cacattttat tcaatgccta tttgtacatg ttactagcaa 60 taaactcttt tatctttaat tttgagaagt tttacaaata cagcaaagca gaatgactaa 120 tagagccggt aaccaggaca cagatttgga aaaataggtc taattggttg ttacactgtg 180 tttatgtcat acatttcgct tatttttatc aaanaaaaat cagaatttat aaaatgttaa 240 ttaaaaggaa aacattctga gtaaatttag tcccgtgttt cttcctccaa atctntttgt 300 tctacactaa caggtcagga taagtatgga tggggaggct ggaaaaaggg catccttccc 360 catgcggtcc ccagagccac cctctccaag caggac 396 <210> SEQ ID NO 150 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 150 acgcctctct tcagttggca cccaaacatc tggattggca aatcagtggc aagaagttcc 60 agcatctgga cttttcagaa ttgatcttaa gtctactgtc atttccagat gcattatttt 120 acaactgtat ccttggaaat atatttctag ggagaatatt attgaagaaa atgttaatag 180 cctgagtcaa atttcagcag acttaccagc atttgtatca gtggtagcaa atgaagccaa 240 actgtatctt gaaaaacctg ttgttccttt aaatatgatg ttgccacaag ctgcattgga 300 gactcattgc agtaatattt ccaatgtgcc acctacaaga gagatacttc aagtctttct 360 tactgatgta cacatgaagg aagtaattca gcagtt 396 <210> SEQ ID NO 151 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 146, 299, 332 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 151 acaaaatgcc cagcctacag agtctgagaa ggaaatttat aatcaggtga atgtagtatt 60 aaaagatgca gaaggcatct tggaggactt gcagtcatac agaggagctg gccacgaaat 120 acgagaggca atccagcatc cagcanatga gaagttgcaa gagaaggcat ggggtgcagt 180 tgttccacta gtaggcaaat taaagaaatt ttacgaattt tctcagaggt tagaagcagc 240 attaagaggt cttctgggag ccttaacaag taccccatat tctcccaccc agcatctana 300 gcgagagcag gctcttgcta aacagtttgc anaaattctt catttcacac tccggtttga 360 tgaactcaag atgacaaatc ctgccataca gaatga 396 <210> SEQ ID NO 152 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 249 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 152 acgcagcgct cggcttcctg gtaattcttc acctcttttc tcagctccct gcagcatggg 60 tgctgggccc tccttgctgc tcgccgccct cctgctgctt ctctccggcg acggcgccgt 120 gcgctgcgac acacctgcca actgcaccta tcttgacctg ctgggcacct gggtcttcca 180 ggtgggctcc agcggttccc agcgcgatgt caactgctcg gttatgggac cacaagaaaa 240 aaaagtagng gtgtaccttc agaagctgga tacagcatat gatgaccttg gcaattctgg 300 ccatttcacc atcatttaca accaaggctt tgagattgtg ttgaatgact acaagtggtt 360 tgcctttttt aagtataaag aagagggcag caaggt 396 <210> SEQ ID NO 153 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 153 ccagagacaa cttcgcggtg tggtgaactc tctgaggaaa aacacgtgcg tggcaacaag 60 tgactgagac ctagaaatcc aagcgttgga ggtcctgagg ccagcctaag tcgcttcaaa 120 atggaacgaa ggcgtttgcg gggttccatt cagagccgat acatcagcat gagtgtgtgg 180 acaagcccac ggagacttgt ggagctggca gggcagagcc tgctgaagga tgaggccctg 240 gccattgccg ccctggagtt gctgcccagg gagctcttcc cgccactctt catggcagcc 300 tttgacggga gacacagcca gaccctgaag gcaatggtgc aggcctggcc cttcacctgc 360 ctccctctgg gagtgctgat gaagggacaa catctt 396 <210> SEQ ID NO 154 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 42, 45, 59, 82 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 154 acagcaaacc tcctcacagc ccactggtcc tcaagagggg cnacntcttc acacatcanc 60 acaactacgc attgcctccc tncactcgga aggactatcc tgctgccaag agggtcaagt 120 tggacagtgt cagagtcctg agacagatca gcaacaaccg aaaatgcacc agccccaggt 180 cctcggacac cgaggagaat gtcaagaggc gaacacacaa cgtcttggag cgccagagga 240 ggaacgagct aaaacggagc ttttttgccc tgcgtgacca gatcccggag ttggaaaaca 300 atgaaaaggc ccccaaggta gttatcctta aaaaagccac agcatacatc ctgtccgtcc 360 aagcagagga gcaaaagctc atttctgaag aggact 396 <210> SEQ ID NO 155 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 15, 17, 202, 280, 339 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 155 tttttttttt tgaananaca ggtctttaat gtacggagtc tcacaaggca caaacaccct 60 caccaggacc aaataaataa ctccacggtt gcaggaaggc gcggtctggg gaggatgcgg 120 catctgagct ctcccagggc tggtgggcga gccgggggtc tgcagtctgt gaggggcctc 180 ctgggtgtgt ccgggcctct anagcgggtc cagtctccag gatggggatc gctcactcac 240 tctccgagtc ggagtagtcc gccacgaggg aggagccgan actgcagggg tgccgcgtgt 300 cgggggtgtc agctgcctcc tgggaggagc ctgctggcna caggggcttg tcctgacggc 360 tcccttcctg ccccctcggg ctgctgcact tggggg 396 <210> SEQ ID NO 156 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 11, 30, 32, 37, 309, 332 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 156 gaaggggggc ngggcagggg cggaatgtan anattantgc catgattgaa gatttaagaa 60 acgtgagatt caggattttc accacatccc catttagtta gcttgctcgt ttggctggtg 120 caaatgccag atggattatg aacaatgaca gtaaattaat gcaacataat caggtaatga 180 tgccaagcgt atctggtgtt ccaggtattg tacctttacc ggaacaaatc agtaaatcca 240 caatccctgg cacctgttag gcagctatta acctagtaaa tgctccccca tcccatctca 300 atcagcaang acaatcaaaa acatttgctt tnagtggcag gaacactggt acatttttac 360 ttgctccaag ggctgtgcca acgctccctc tctctg 396 <210> SEQ ID NO 157 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 121, 202, 204, 255, 314, 332, 368 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 157 tttttttttt tttttgggga atgtaaatct tttattaaaa cagttgtctt tccacagtag 60 taaagctttg gcacatacag tataaaaaat aatcacccac cataattata ccaaattcct 120 nttatcaact gcatactaag tgttttcaat acaatttttt ccgtataaaa atactgggaa 180 aaattgataa ataacaggta ananaaagat atttctaggc aattactagg atcatttgga 240 aaaagtgagt actgnggata tttaaaatat cacagtaaca agatcatgct tgttcctaca 300 gtattgcggg ccanacactt aagtgaaagc anaagtgttt gggtgacttt cctacttaaa 360 attttggnca tatcatttca aaacatttgc atcttg 396 <210> SEQ ID NO 158 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 158 tttccgaaga cgggcagctt cagagaagag gattattcgg gagattgctg gtgtggccca 60 tagactcttt ggcatagact ctttcgcagg cagccactct gagtgtggcc agttctataa 120 ccatccccaa actagctgga gcctgatgga taggaacggg tagtctgtcc tcttccccat 180 aaaaatgttc caaaaagtta tctccagaga gagtccctta tgaagacagt tgccaagctg 240 tattctcatt ctttaaacca atacccaggt cagggctagt tcacactagc actgttaggg 300 acatggtgtg gctagaaatg aattgagtgt gacttctccc tacaacccca ggcccaggga 360 taggaggagg cagaggggtg cctggagttt ctgcac 396 <210> SEQ ID NO 159 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 159 tccgcgcgtt gggaggtgta gcgcggctct gaacgcgctg agggccgttg agtgtcgcag 60 gcggcgaggg cgcgagtgag gagcagaccc aggcatcgcg cgccgagaag gccgggcgtc 120 cccacactga aggtccggaa aggcgacttc cgggggcttt ggcacctggc ggaccctccc 180 ggagcgtcgg cacctgaacg cgaggcgctc cattgcgcgt gcgcgttgag gggcttcccg 240 cacctgatcg cgagacccca acggctggtg gcgtcgcctg cgcgtctcgg ctgagctggc 300 catggcgcag ctgtgcgggc tgaggcggag ccgggcgttt ctcgccctgc tgggatcgct 360 gctcctctct ggggtcctgg cggccgaccg agaacg 396 <210> SEQ ID NO 160 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 96, 102, 122, 124, 129, 146, 148, 184, 189, 196, 205, 208, 229, 246, 259, 261, 269, 272, 281, 297, 305, 308, 327, 331, 337, 338, 339, 343, 346, 354, 366, 367, 369, 378, 379, 380, 381, 391, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 160 ggaaaccttc tcaactaaga gaacatcatt tctggcaaac tatttttgtt agctcacaat 60 atatgtcgta cactctacaa tgtaaatagc actganccac ancttacaga aggtaaaaag 120 angnataana acttccttta caaaanantt cctgttgttc ttaatactcc ccattgctta 180 tganaattnt ctatangtct ctcangantg ttcgcaccca tttcttttnt aacttctact 240 aaaaanccat ttacattgna nagtgtacna cntatatttg ngagctaaca aaaaatngtt 300 ttccnganat gatgttcttt tagtttnaga nggttcnnnc aanttnctac tccngcccgc 360 cactgnncnc cacatttnnn naattacacc ncacng 396 <210> SEQ ID NO 161 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 271, 273, 325, 364 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 161 tttttgtttg attattttta ttataatgaa attaaactta tgactattac agtatgctca 60 gcttaaaaca tttatgagta ctgcaaggac taacagaaac aggaaaaatc ctactaaaaa 120 tatttgttga tgggaaatca ttgtgaaagc aaacctccaa atattcattt gtaagccata 180 agaggataag cacaaccata tgggaggaga taaccagtct ctcccttcat atatattctt 240 ttttatttct tggtatacct tcccaaaaca nanacattca acagtagtta gaatggccat 300 ctcccaacat tttaaaaaaa ctgcnccccc caatgggtga acaaagtaaa gagtagtaac 360 ctanagttca gctgagtaag ccactgtgga gcctta 396 <210> SEQ ID NO 162 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 33, 38, 51, 62, 71, 72, 88, 97, 98, 100, 106, 142, 155, 160, 161, 163, 168, 170, 174, 183, 190, 194, 203, 214, 216, 231, 232, 241, 242, 252, 258, 260, 264, 265, 267, 276, 278, 282, 287, 289, 292, 295, 297, 301, 311, 319, 322, 325 <223> OTHER INFORMATION: n = A,T,C or G <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 330, 337, 341, 342, 347, 348, 354, 356, 361, 367, 368, 375, 379, 385, 391, 394, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 162 tttttttttt tttttttttt tttttttttt ttnggggncc aaattttttt ntttgaagga 60 angggacaaa nnaaaaaact taaggggntg ttttggnncn acttanaaaa aagggaaagg 120 aaaccccaac atgcatgccc tnccttgggg accanggaan ncnccccncn ggtntgggga 180 aantaacccn aggnttaact ttnattatca ctgncnccca gggggggctt nnaaaaaaaa 240 nnttccccca anccaaantn gggnncnccc attttncnca anttggncnc cnggncnccc 300 nattttttga ngggtttcnc cngcncattn agggaanggg nntcaannaa accncncaaa 360 ngggggnnat ttttntcang ggccnatttg ngcnnt 396 <210> SEQ ID NO 163 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 163 cactgtccgg ctctaacaca gctattaagt gctacctgcc tctcaggcac tctcctcgcc 60 cagtttctga ggtcagacga gtgtctgcga tgtcttcccg cactctattc ccccagcctc 120 tttctgcttt catgctcagc acatcatctt cctaggcagt ctcttcccca aagtctcacc 180 ttttcttcca atagaaaatt ccgcttgacc tttggtgcac tgcccacttc ccagctccac 240 tggcccaagt ctgagccgga ggcccttgtt ttgggggcgg ggggagagtt ggatgtgatt 300 gcccttgaag aacaaggctg acctgagagg ttcctggcgc cctgaggtgg ctcagcacct 360 gcccagggta ggcctggcat gaggggttag gtcagc 396 <210> SEQ ID NO 164 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 164 gacacgcggc ggtgtcctgt gttggccatg gccgactacc tgattagtgg gggcacgtcc 60 tacgtgccag acgacggact cacagcacag cagctcttca actgcggaga cggcctcacc 120 tacaatgact ttctcattct ccctgggtac atcgacttca ctgcagacca ggtggacctg 180 acttctgctc tgaccaagaa aatcactctt aagaccccac tggtttcctc tcccatggac 240 acagtcacag aggctgggat ggccatagca atggcgctta caggcggtat tggcttcatc 300 caccacaact gtacacctga attccaggcc aatgaagttc ggaaagtgaa gaaatatgaa 360 cagggattca tcacagaccc tgtggtcctc agcccc 396 <210> SEQ ID NO 165 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 29, 33, 55, 57, 65, 77, 82, 87, 98, 101, 103, 114, 118, 124, 169, 171, 173, 183, 186, 188, 216, 219, 227, 230, 242, 243, 245, 252, 265, 273, 290, 296, 321, 324, 332, 338, 340, 342, 345, 359, 372, 380 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 165 tttttttttt tttttttttt ttttttcang ggncactgag gctttttatt ttgancncaa 60 aaccnccggg gatctancct gnggccnccc cggaaatnac ncnaggctca catnactnta 120 aacncttggg ggaaagggag gcaaaaaaaa caatgacttg ggccaattnc ncnactgcaa 180 agntananct gccaacaggg ctccagggag cttggnttnt gtaaaanttn taaggaagcg 240 gnncnaactc cncggggggg gggcnctaac tancagggac ccctgcaagn gttggncggg 300 ggcctcaacc tgcctgagct nacncaaggg gnggggtntn tntanccaac aggggaccna 360 agggcttgcc tncccacagn ttacttggcc aagggg 396 <210> SEQ ID NO 166 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 151, 255 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 166 ttttttcaaa ttcagagcat ttttattaaa agaacaaaat attaaggcac aaaatacatc 60 aatttttcaa atgaaaaccc ttcaaacggt tatgtcctac attcaacgaa acttcttcca 120 aattacggaa taatttaact ttttaaaata naaaaataca agttcttaaa tgcctaaaat 180 ttctccccaa ataaatgttt tcttagtttt aatgaagtct cttcatgcag tactgagctc 240 caatattata atgtncactt ccttaaaaat ctagttttgc cacttatata cattcaatat 300 gtttaaccag tatattaacc agtatattaa ccaatatgtt aaacttcttt taagtataag 360 gcttggtatt ttgtattgct tattgcatgc tttgat 396 <210> SEQ ID NO 167 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 167 tggcggcagc ggcggtggcg gtggctgagc agaggacccg gcgggcggcc tcgcgggtca 60 ggacacaatg tttgcacgag gactgaagag gaaatgtgtt ggccacgagg aagacgtgga 120 gggagccctg gccggcttga agacagtgtc ctcatacagc ctgcagcggc agtcgctcct 180 ggacatgtct ctggtgaagt tgcagctttg ccacatgctt gtggagccca atctgtgccg 240 ctcagtcctc attgccaaca cggtccggca gatccaagag gagatgacgc aggatgggac 300 gtggcgcaca gtggcacccc aggctgcaga gcgggcgccg ctcgaccgct tggtctccac 360 ggagatcctg tgccgtgcag cgtgggggca agaggg 396 <210> SEQ ID NO 168 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 168 taggatggta agagtattat aaggattggt acaaggcatg atgagtcctt ttgcttttag 60 gcttttgact tctggtttta gactttcttt agcttctgtt gttagacaac attgtgcaag 120 cttggttttt ataagtttgc atggattaaa ctgaacttaa tgaaattgtc cctcccccca 180 aattctcagc acaattttta ggcccacaag gagtcaagca cctcaaggag atcttcagtt 240 tgaacttggt gtagacacag ggatactgat gaatcaatat tcaaattagc tgttacctac 300 ttaagaaaga gaggagacct tggggatttc gaggaagggt tcataaggga gattttagct 360 gagaaatacc atttgcacag tcaatcactt ctgacc 396 <210> SEQ ID NO 169 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 16, 58, 76, 84, 99, 111, 114, 124, 136, 140, 161, 167, 184, 189, 204, 206, 210, 228, 230, 232, 243, 275, 277, 289, 301, 303, 312, 319, 321, 323, 325, 333, 345, 349, 355, 359, 364, 365, 372, 375, 377, 379, 383, 387, 389, 394, 396 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 169 tttttttttt tttcanaatt aaattcttta atacaaaatg cttttttttt tttaaaanat 60 atctgtattt ctttgncgtt gttnaaaaat aaatatgtnc tacggaatat ntcnaaaaac 120 tgcnctaaaa acaaanacgn gatgttaata tcttttcccc ncaattntta cggataaaca 180 gtanccccna taaataaatg atancnaatn ttaaaattaa aaaagganan anatttagta 240 tgnaaaattc tctatttttt cttggtttgg ttttncntat aaaaaacana atagcaatgt 300 ntnttttatc anaatcccnt ntntncctaa acnttttttt ttttntttnc ccccnaatnc 360 aagnngccaa anatntntnt agnatgnana tgtntn 396 <210> SEQ ID NO 170 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 170 tgagaagtac catgccgctt ctgcagagga acaggcaacc atcgaacgca acccctacac 60 catcttccat caagcactga aaaactgtga gcctatgatt gggctggtac ccatcctcaa 120 gggaggccgt ttctaccagg tccctgtacc cctacccgac cggcgtcgcc gcttcctagc 180 catgaagtgg atgatcactg agtgccggga taaaaagcac cagcggacac tgatgccgga 240 gaagctgtca cacaagctgc tggaggcttt ccataaccag ggccccgtga tcaagaggaa 300 gcatgacttg cacaagatgg cagaggccaa ccgtgccctg gcccactacc gctggtggta 360 gagtctccag gaggagccca gggccctctg cgcaag 396 <210> SEQ ID NO 171 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 133, 224, 260, 264, 268, 279, 283, 317, 322, 338, 360, 370, 371, 378 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 171 ggtcctcgtc gtggtgagcg cagccactca ggctggtcct gggggtgggg ctgtagggga 60 aagtgctaaa gccgctgagt gaagtaagaa ctctgctaga gaggaaaatg ggcttgcttt 120 catcatcatc ctnctcagct ggtggggtca agtgggaagt tctgtcactg ggatctggtt 180 cagtgtctca agaccttgcc ccaccacgga aagccttttt cacntacccc aaaggacttg 240 gagagatgtt agaagatggn tctnaaanat tcctctgcna atntgttttt agctatcaag 300 tggcttcccc ccttaancag gnaaaacatg atcagcangt tgctcggatg gaaaaactan 360 cttggtttgn naaaaaanct ggaggcttga caatgg 396 <210> SEQ ID NO 172 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 239, 242, 244, 246, 249, 257, 260, 314, 329, 355, 372, 378, 385, 387, 388, 395 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 172 agccttgggc caccctcttg gagcatctgg ctgtcgaatt cttgtgaccc tgttacacac 60 actggagaga atgggcagaa gtcgtggtgt tgcagccctg tgcattgggg gtgggatggg 120 aatagcaatg tgtgttcaga gagaatgaat tgcttaaact ttgaacaacc tcaatttctt 180 tttaaactaa taaagtacta ggttgcaata tgtgaaaaaa aaaaaaaaag ggcggccgnt 240 cnantntana gggcccnttn aaacccgttg atcaacctcg actgtgcctt ctagttgcca 300 gccatctgtt gttngcccct cccccgtgnc tttcttgacc ttgaaagggg ccccncccct 360 gtctttccta anaaaaanga agaantnncc ttccnt 396 <210> SEQ ID NO 173 <211> LENGTH: 396 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 209, 210, 232, 244, 270, 275, 284, 341, 343, 349, 359, 364, 368, 376, 380, 382, 388, 389, 390, 392 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 173 aagcatgtgg atatgtttag ctacgtttac tcacagccag cgaactgaca ttaaaataac 60 taacaaacag attcttttat gtgatgctgg aactcttgac agctataatt attattcaga 120 aatgactttt tgaaagtaaa agcagcataa agaatttgtc acaggaaggc tgtctcagat 180 aaattatggt aaaattttgc aggggacann ctttttaaga cttgcacaat tnccggatcc 240 tgcnctgact ttggaaaagg catatatgtn ctagnggcat gganaatgcc ccatactcat 300 gcatgcaaat taaacaacca agtttgaatc tttttggggg ngngctatnc tttaacccng 360 tacnggcntt attatntaan gnccctgnnn cntgtg 396 <210> SEQ ID NO 174 <211> LENGTH: 924 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 174 cctgacgacc cggcgacggc gacgtctctt ttgactaaaa gacagtgtcc agtgctccag 60 cctaggagtc tacggggacc gcctcccgcg ccgccaccat gcccaacttc tctggcaact 120 ggaaaatcat ccgatcggaa aacttcgagg aattgctcaa agtgctgggg gtgaatgtga 180 tgctgaggaa gattgctgtg gctgcagcgt ccaagccagc agtggagatc aaacaggagg 240 gagacacttt ctacatcaaa acctccacca ccgtgcgcac cacagagatt aacttcaagg 300 ttggggagga gtttgaggag cagactgtgg atgggaggcc ctgtaagagc ctggtgaaat 360 gggagagtga gaataaaatg gtctgtgagc agaagctcct gaagggagag ggccccaaga 420 cctcgtggac cagagaactg accaacgatg gggaactgat cctgaccatg acggcggatg 480 acgttgtgtg caccagggtc tacgtccgag agtgagtggc cacaggtaga accgcggccg 540 aagcccacca ctggccatgc tcaccgccct gcttcactgc cccctccgtc ccaccccctc 600 cttctaggat agcgctcccc ttaccccagt cacttctggg ggtcactggg atgcctcttg 660 cagggtcttg ctttctttga cctcttctct cctcccctac accaacaaag aggaatggct 720 gcaagagccc agatcaccca ttccgggttc actccccgcc tccccaagtc agcagtccta 780 gccccaaacc agcccagagc agggtctctc taaaggggac ttgagggcct gagcaggaaa 840 gactggccct ctagcttcta ccctttgtcc ctgtagccta tacagtttag aatatttatt 900 tgttaatttt attaaaatgc ttta 924 <210> SEQ ID NO 175 <211> LENGTH: 3321 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 175 atgaagattt tgatacttgg tatttttctg tttttatgta gtaccccagc ctgggcgaaa 60 gaaaagcatt attacattgg aattattgaa acgacttggg attatgcctc tgaccatggg 120 gaaaagaaac ttatttctgt tgacacggaa cattccaata tctatcttca aaatggccca 180 gatagaattg ggagactata taagaaggcc ctttatcttc agtacacaga tgaaaccttt 240 aggacaacta tagaaaaacc ggtctggctt gggtttttag gccctattat caaagctgaa 300 actggagata aagtttatgt acacttaaaa aaccttgcct ctaggcccta cacctttcat 360 tcacatggaa taacttacta taaggaacat gagggggcca tctaccctga taacaccaca 420 gattttcaaa gagcagatga caaagtatat ccaggagagc agtatacata catgttgctt 480 gccactgaag aacaaagtcc tggggaagga gatggcaatt gtgtgactag gatttaccat 540 tcccacattg atgctccaaa agatattgcc tcaggactca tcggaccttt aataatctgt 600 aaaaaagatt ctctagataa agaaaaagaa aaacatattg accgagaatt tgtggtgatg 660 ttttctgtgg tggatgaaaa tttcagctgg tacctagaag acaacattaa aacctactgc 720 tcagaaccag agaaagttga caaagacaac gaagacttcc aggagagtaa cagaatgtat 780 tctgtgaatg gatacacttt tggaagtctc ccaggactct ccatgtgtgc tgaagacaga 840 gtaaaatggt acctttttgg tatgggtaat gaagttgatg tgcacgcagc tttctttcac 900 gggcaagcac tgactaacaa gaactaccgt attgacacaa tcaacctctt tcctgctacc 960 ctgtttgatg cttatatggt ggcccagaac cctggagaat ggatgctcag ctgtcagaat 1020 ctaaaccatc tgaaagccgg tttgcaagcc tttttccagg tccaggagtg taacaagtct 1080 tcatcaaagg ataatatccg tgggaagcat gttagacact actacattgc cgctgaggaa 1140 atcatctgga actatgctcc ctctggtata gacatcttca ctaaagaaaa cttaacagca 1200 cctggaagtg actcagcggt gttttttgaa caaggtacca caagaattgg aggctcttat 1260 aaaaagctgg tttatcgtga gtacacagat gcctccttca caaatcgaaa ggagagaggc 1320 cctgaagaag agcatcttgg catcctgggt cctgtcattt gggcagaggt gggagacacc 1380 atcagagtaa ccttccataa caaaggagca tatcccctca gtattgagcc gattggggtg 1440 agattcaata agaacaacga gggcacatac tattccccaa attacaaccc ccagagcaga 1500 agtgtgcctc cttcagcctc ccatgtggca cccacagaaa cattcaccta tgaatggact 1560 gtccccaaag aagtaggacc cactaatgca gatcctgtgt gtctagctaa gatgtattat 1620 tctgctgtgg atcccactaa agatatattc actgggctta ttgggccaat gaaaatatgc 1680 aagaaaggaa gtttacatgc aaatgggaga cagaaagatg tagacaagga attctatttg 1740 tttcctacag tatttgatga gaatgagagt ttactcctgg aagataatat tagaatgttt 1800 acaactgcac ctgatcaggt ggataaggaa gatgaagact ttcaggaatc taataaaatg 1860 cactccatga atggattcat gtatgggaat cagccgggtc tcactatgtg caaaggagat 1920 tcggtcgtgt ggtacttatt cagcgccgga aatgaggccg atgtacatgg aatatacttt 1980 tcaggaaaca catatctgtg gagaggagaa cggagagaca cagcaaacct cttccctcaa 2040 acaagtctta cgctccacat gtggcctgac acagagggga cttttaatgt tgaatgcctt 2100 acaactgatc attacacagg cggcatgaag caaaaatata ctgtgaacca atgcaggcgg 2160 cagtctgagg attccacctt ctacctggga gagaggacat actatatcgc agcagtggag 2220 gtggaatggg attattcccc acaaagggag tgggaaaagg agctgcatca tttacaagag 2280 cagaatgttt caaatgcatt tttagataag ggagagtttt acataggctc aaagtacaag 2340 aaagttgtgt atcggcagta tactgatagc acattccgtg ttccagtgga gagaaaagct 2400 gaagaagaac atctgggaat tctaggtcca caacttcatg cagatgttgg agacaaagtc 2460 aaaattatct ttaaaaacat ggccacaagg ccctactcaa tacatgccca tggggtacaa 2520 acagagagtt ctacagttac tccaacatta ccaggtgaaa ctctcactta cgtatggaaa 2580 atcccagaaa gatctggagc tggaacagag gattctgctt gtattccatg ggcttattat 2640 tcaactgtgg atcaagttaa ggacctctac agtggattaa ttggccccct gattgtttgt 2700 cgaagacctt acttgaaagt attcaatccc agaaggaagc tggaatttgc ccttctgttt 2760 ctagtttttg atgagaatga atcttggtac ttagatgaca acatcaaaac atactctgat 2820 caccccgaga aagtaaacaa agatgatgag gaattcatag aaagcaataa aatgcatgct 2880 attaatggaa gaatgtttgg aaacctacaa ggcctcacaa tgcacgtggg agatgaagtc 2940 aactggtatc tgatgggaat gggcaatgaa atagacttac acactgtaca ttttcacggc 3000 catagcttcc aatacaagca caggggagtt tatagttctg atgtctttga cattttccct 3060 ggaacatacc aaaccctaga aatgtttcca agaacacctg gaatttggtt actccactgc 3120 catgtgaccg accacattca tgctggaatg gaaaccactt acaccgttct acaaaatgaa 3180 gacaccaaat ctggctgaat gaaataaatt ggtgataagt ggaaaaaaga gaaaaaccaa 3240 tgattcataa caatgtatgt gaaagtgtaa aatagaatgt tactttggaa tgactataaa 3300 cattaaaaga gactggagca t 3321 <210> SEQ ID NO 176 <211> LENGTH: 487 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 176 gaaatacttt ctgtcttatt aaaattaata aattattggt ctttacaaga cttggataca 60 ttacagcaga catggaaata taattttaaa aaatttctct ccaacctcct tcaaattcag 120 tcaccactgt tatattacct tctccaggaa ccctccagtg gggaaggctg cgatattaga 180 tttccttgta tgcaaagttt ttgttgaaag ctgtgctcag aggaggtgag aggagaggaa 240 ggagaaaact gcatcataac tttacagaat tgaatctaga gtcttccccg aaaagcccag 300 aaacttctct gcagtatctg gcttgtccat ctggtctaag gtggctgctt cttccccagc 360 catgagtcag tttgtgccca tgaataatac acgacctgtt atttccatga ctgctttact 420 gtatttttaa ggtcaatata ctgtacattt gataataaaa taatattctc ccaaaaaaaa 480 aaaaaaa 487 <210> SEQ ID NO 177 <211> LENGTH: 3999 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 177 caagattcca catttgatgg ggtgactgac aaacccatct tagactgctg tgcctgcgga 60 actgccaagt acagactcac attttatggg aattggtccg agaagacaca cccaaaggat 120 taccctcgtc gggccaacca ctggtctgcg atcatcggag gatcccactc caagaattat 180 gtactgtggg aatatggagg atatgccagc gaaggcgtca aacaagttgc agaattgggc 240 tcacccgtga aaatggagga agaaattcga caacagagtg atgaggtcct caccgtcatc 300 aaagccaaag cccaatggcc agcctggcag cctctcaacg tgagagcagc accttcagct 360 gaattttccg tggacagaac gcgccattta atgtccttcc tgaccatgat gggccctagt 420 cccgactgga acgtaggctt atctgcagaa gatctgtgca ccaaggaatg tggctgggtc 480 cagaaggtgg tgcaagacct gattccctgg gacgctggca ccgacagcgg ggtgacctat 540 gagtcaccca acaaacccac cattccccag gagaaaatcc ggcccctgac cagcctggac 600 catcctcaga gtcctttcta tgacccagag ggtgggtcca tcactcaagt agccagagtt 660 gtcatcgaga gaatcgcacg gaagggtgaa caatgcaata ttgtacctga caatgtcgat 720 gatattgtag ctgacctggc tccagaagag aaagatgaag atgacacccc tgaaacctgc 780 atctactcca actggtcccc atggtccgcc tgcagctcct ccacctgtga caaaggcaag 840 aggatgcgac agcgcatgct gaaagcacag ctggacctca gcgtcccctg ccctgacacc 900 caggacttcc agccctgcat gggccctggc tgcagtgacg aagacggctc cacctgcacc 960 atgtccgagt ggatcacctg gtcgccctgc agcatctcct gcggcatggg catgaggtcc 1020 cgggagaggt atgtgaagca gttcccggag gacggctccg tgtgcacgct gcccactgag 1080 gaaacggaga agtgcacggt caacgaggag tgctctccca gcagctgcct gatgaccgag 1140 tggggcgagt gggacgagtg cagcgccacc tgcggcatgg gcatgaagaa gcggcaccgc 1200 atgatcaaga tgaaccccgc agatggctcc atgtgcaaag ccgagacatc acaggcagag 1260 aagtgcatga tgccagagtg ccacaccatc ccatgcttgc tgtccccatg gtccgagtgg 1320 agtgactgca gcgtgacctg cgggaagggc atgcgaaccc gacagcggat gctcaagtct 1380 ctggcagaac ttggagactg caatgaggat ctggagcagg tggagaagtg catgctccct 1440 gaatgcccca ttgactgtga gctcaccgag tggtcccagt ggtcggaatg taacaagtca 1500 tgtgggaaag gccacgtgat tcgaacccgg atgatccaaa tggagcctca gtttggaggt 1560 gcaccctgcc cagagactgt gcagcgaaaa aagtgccgca tccgaaaatg ccttcgaaat 1620 ccatccatcc aaaagctacg ctggagggag gcccgagaga gccggcggag tgagcagctg 1680 aaggaagagt ctgaagggga gcagttccca ggttgtagga tgcgcccatg gacggcctgg 1740 tcagaatgca ccaaactgtg cggaggtgga attcaggaac gttacatgac tgtaaagaag 1800 agattcaaaa gctcccagtt taccagctgc aaagacaaga aggagatcag agcatgcaat 1860 gttcatcctt gttagcaagg gtacgagttc cccagggctg cactctagat tccagagtca 1920 ccaatggctg gattatttgc ttgtttaaga caatttaaat tgtgtacgct agttttcatt 1980 tttgcagtgt ggttcgccca gtagtcttgt ggatgccaga gacatccttt ctgaatactt 2040 cttgatgggt acaggctgag tggggcgccc tcacctccag ccagcctctt cctgcagagg 2100 agtagtgtca gccaccttgt actaagctga aacatgtccc tctggagctt ccacctggcc 2160 agggaggacg gagactttga cctactccac atggagaggc aaccatgtct ggaagtgact 2220 atgcctgagt cccagggtgc ggcaggtagg aaacattcac agatgaagac agcagattcc 2280 ccacattctc atctttggcc tgttcaatga aaccattgtt tgcccatctc ttcttagtgg 2340 aactttaggt ctcttttcaa gtctcctcag tcatcaatag ttcctgggga aaaacagagc 2400 tggtagactt gaagaggagc attgatgttg ggtggctttt gttctttcac tgagaaattc 2460 ggaatacatt tgtctcaccc ctgatattgg ttcctgatgc ccccccaaca aaaataaata 2520 aataaattat ggctgcttta tttaaatata aggtagctag tttttacacc tgagataaat 2580 aataagctta gagtgtattt ttcccttgct tttgggggtt cagaggagta tgtacaattc 2640 ttctgggaag ccagccttct gaactttttg gtactaaatc cttattggaa ccaagacaaa 2700 ggaagcaaaa ttggtctctt tagagaccaa tttgcctaaa ttttaaaatc ttcctacaca 2760 catctagacg ttcaagtttg caaatcagtt tttagcaaga aaacattttt gctatacaaa 2820 cattttgcta agtctgccca aagccccccc aatgcattcc ttcaacaaaa tacaatctct 2880 gtactttaaa gttattttag tcatgaaatt ttatatgcag agagaaaaag ttaccgagac 2940 agaaaacaaa tctaagggaa aggaatatta tgggattaag ctgagcaagc aattctggtg 3000 gaaagtcaaa cctgtcagtg ctccacacca gggctgtggt cctcccagac atgcatagga 3060 atggccacag gtttacactg ccttcccagc aattataagc acaccagatt cagggagact 3120 gaccaccaag ggatagtgta aaaggacatt ttctcagttg ggtccatcag cagtttttct 3180 tcctgcattt attgttgaaa actattgttt catttcttct tttataggcc ttattactgc 3240 ttaatccaaa tgtgtaccat tggtgagaca catacaatgc tctgaataca ctacgaattt 3300 gtattaaaca catcagaata tttccaaata caacatagta tagtcctgaa tatgtacttt 3360 taacacaaga gagactattc aataaaaact cactgggtct ttcatgtctt taagctaagt 3420 aagtgttcag aaggttcttt tttatattgt cctccacctc catcattttc aataaaagat 3480 agggcttttg ctcccttgtt cttggaggga ccattattac atctctgaac tacctttgta 3540 tccaacatgt tttaaatcct taaatgaatt gctttctccc aaaaaaagca caatataaag 3600 aaacacaaga tttaattatt tttctacttg gggggaaaaa agtcctcatg tagaagcacc 3660 cacttttgca atgttgttct aagctatcta tctaactctc agcccatgat aaagttcctt 3720 aagctggtga ttcctaatca aggacaagcc accctagtgt ctcatgtttg tatttggtcc 3780 cagttgggta cattttaaaa tcctgatttt ggagacttaa aaccaggtta atggctaaga 3840 atgggtaaca tgactcttgt tggattgtta ttttttgttt gcaatgggga atttataaga 3900 agcatcaagt ctctttctta ccaaagtctt gttaggtggt ttatagttct tttggctaac 3960 aaatcatttt ggaaataaag attttttact acaaaaatg 3999 <210> SEQ ID NO 178 <211> LENGTH: 1069 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 178 aaaaaagatg aataaatgaa taagagagat gaataaacaa atttacatta catgtgatag 60 ttatcatggt atggccttca tgacaagatg gatgagaata tcactgatag gatattagcc 120 ttctttcata tctttatatt gaaatatggg ctttacttca atttgaaggt ctttcatgaa 180 caataaaaga gagtagaagg actgtctgag aaggcaggag acatataaaa cagatgactg 240 aaagactgac tagctcctgg aaagggaaac atttggaaca tccagagtaa gggcaaatgg 300 gcttctacca gcacaacaaa gagcctccag gtggcaacat ggaagcaggt tatcagagaa 360 aataaatgtg caaattcctt atttacaatg actcacttaa ccccacaaac atgtttcact 420 gctgccttcc ccagttgtcg cttatgtact gttgttacct ttcagttaca tgcctttgat 480 cctaaaattc tctacttttg gtgccttatc agttctttgc aatctgcctg tggttatcag 540 cacttaaagc acaattttga aggggaaaaa aatgataatc accttagtcc caaagaaata 600 atttgtcaaa ctgccttatt agtattaaaa acagacacac tgaatgaagt agcatgatac 660 gcatatatcc tactcagtat cattggcctt ttatcaaatg gggaaactat acttttgtat 720 tacatagttt tagaaatcga aagttagaga ctctttataa gtaatgtcaa ggaacagtaa 780 tttaaaaaca aagttctaac aaatatattg tttgcttaat cacaatgccc tcaacttgta 840 tttgaataac taaataggac atgtcttcct tggagctgtg ggcattagtt cagaagcact 900 acctgcatct taattttcaa aacttaagtt ttattagcaa atcctcttct ctgtaagact 960 tagctatgaa gtggtatatt ttttccaaat atttttctga aaacatttgt tgttgtaact 1020 gcacaataaa agtccagttg caattaaaaa aaaaaaaaaa aaaaaaaaa 1069 <210> SEQ ID NO 179 <211> LENGTH: 1817 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 179 tgctattctg ccaaaagaca atttctagag tagttttgaa tgggttgatt tcccccactc 60 ccacaaactc tgaagccagt gtctagctta ctaaaaaaag agttgtatat aatatttaag 120 atgctgagta tttcatagga aagctgaatg ctgctgtaaa gtgctcttta agtctttttt 180 ttttttaatc cccttctaat gaatgaaact aggggaattt caggggacag agatgggatt 240 tgttgtatga taaactgtat gtagttttta gtctttctgt tttgagaagc agtggttggg 300 gcatttttaa gatggctggc tactcttgtt ttccctcatg ataataaatt tgtcataact 360 cagtaacatg aacttgcccc tagaggtagt tgttaataat tttgaaatat taaggtcttg 420 ccaagcttct gatgattcac acctgtacta ctgattatta agcaggacag actgagcttt 480 ctgttgcaaa taccttggag gagaaagtaa tttctaaata tacagagagg taacttgact 540 atatatgttg catcctgtgc ctcccttcat attaatattt gataaagatt ttaatttatg 600 taaaacttct aaagcagaat caaagctcct cttggggaaa tggcaagtct ttaggatagg 660 caagaccctg tatgaatagt accaaagcat taccgcatgg tagagaacac actcgattaa 720 aaatgttaag ctatctgaaa aataaaatgt gcaagtcttc aggatggcac aaaacaaagg 780 ttaatgcttc ttggggcaca tttcttagag ggcttgctga gtgtgtaaat ataatcgact 840 tttgtttgtg ttacatgact tctgtgactt cattgaaaat ctgcacaatt cagtttcagc 900 tctggattac ttcagttgac ctttgtgaag gtttttatct gtgtagaatg ggtgtttgac 960 ttgttttagc ctattaaatt tttattttct ttcactctgt attaaaagta aaacttacta 1020 aaagaaaaga ggtttgtgtt cacattaaat ggttttggtt tggcttcttt tagtcaggct 1080 ttctgaacat tgagatatcc tgaacttaga gctcttcaat cctaagattt tcatgaaaag 1140 cctctcactt gaacccaaac cagagtactc ttactgcctc ttttctaaat gttcaggaaa 1200 agcattgcca gttcagtctt ttcaaaatga gggagaaaca tttgcctgcc ttgtaataac 1260 aagactcagt gcttattttt taaactgcat tttaaaaatt ggatagtata ataacaataa 1320 ggagtaagcc accttttata ggcaccctgt agttttatag ttcttaatct aaacatttta 1380 tatttccttc ttttggaaaa aacctacatg ctacaagcca ccatatgcac agactataca 1440 gtgagttgag ttggctctcc cacagtcttt gaggtgaatt acaaaagtcc agccattatc 1500 atcctcctga gttatttgaa atgatttttt ttgtacattt tggctgcagt attggtggta 1560 gaatatacta taatatggat catctctact tctgtattta tttatttatt actagacctc 1620 aaccacagtc ttctttttcc ccttccacct ctctttgcct gtaggatgta ctgtatgtag 1680 tcatgcactt tgtattaata tattagaaat ctacagatct gttttgtact ttttatactg 1740 ttggatactt ataatcaaaa cttttactag ggtattgaat aaatctagtc ttactagaaa 1800 aaaaaaaaaa aaaaaaa 1817 <210> SEQ ID NO 180 <211> LENGTH: 2382 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 180 acttttattg gaagcagcag ccacatccct gcatgatttg cattgcaata caaccataac 60 cgggcagcca ctcctgagtg ataaccagta taacataaac gtagcagcct caatttttgc 120 ctttatgacg acagcttgtt atggttgcag tttgggtctg gctttacgaa gatggcgacc 180 gtaacactcc ttagaaactg gcagtcgtat gttagtttca cttgtctact ttatatgtct 240 gatcaatttg gataccattt tgtccagatg caaaaacatt ccaaaagtaa tgtgtttagt 300 agagagagac tctaagctca agttctggtt tatttcatgg atggaatgtt aattttatta 360 tgatattaaa gaaatggcct tttattttac atctctcccc tttttccctt tcccccttta 420 ttttcctcct tttctttctg aaagtttcct tttatgtcca taaaatacaa atatattgtt 480 cataaaaaat tagtatccct tttgtttggt tgctgagtca cctgaacctt aattttaatt 540 ggtaattaca gcccctaaaa aaaacacatt tcaaataggc ttcccactaa actctatatt 600 ttagtgtaaa ccaggaattg gcacactttt tttagaatgg gccagatggt aaatatttat 660 gcttcacggt ccatacagtc tctgtcacaa ctattcagtt ctgctagtat agcgtgaaag 720 cagctataca caatacagaa atgaatgagt gtggttatgt tctaataaaa cttatttata 780 aaaacaaggg gaggctgggt ttagcctgtg ggccatagtt tgtcaaccac tggtgtaaaa 840 ccttagttat atatgatctg cattttcttg aactgatcat tgaaaactta taaacctaac 900 agaaaagcca cataatattt agtgtcatta tgcaataatc acattgcctt tgtgttaata 960 gtcaaatact tacctttgga gaatacttac ctttggagga atgtataaaa tttctcaggc 1020 agagtcctgg atataggaaa aagtaattta tgaagtaaac ttcagttgct taatcaaact 1080 aatgatagtc taacaactga gcaagatcct catctgagag tgcttaaaat gggatcccca 1140 gagaccatta accaatactg gaactggtat ctagctactg atgtcttact ttgagtttat 1200 ttatgcttca gaatacagtt gtttgccctg tgcatgaata tacccatatt tgtgtgtgga 1260 tatgtgaagc ttttccaaat agagctctca gaagaattaa gtttttactt ctaattattt 1320 tgcattactt tgagttaaat ttgaatagag tattaaatat aaagttgtag attcttatgt 1380 gtttttgtat tagcccagac atctgtaatg tttttgcact ggtgacagac aaaatctgtt 1440 ttaaaatcat atccagcaca aaaactattt ctggctgaat agcacagaaa agtattttaa 1500 cctacctgta gagatcctcg tcatggaaag gtgccaaact gttttgaatg gaaggacaag 1560 taagagtgag gccacagttc ccaccacacg agggcttttg tattgttcta ctttttcagc 1620 cctttacttt ctggctgaag catccccttg gagtgccatg tataagttgg gctattagag 1680 ttcatggaac atagaacaac catgaatgag tggcatgatc cgtgcttaat gatcaagtgt 1740 tacttatcta ataatcctct agaaagaacc ctgttagatc ttggtttgtg ataaaaatat 1800 aaagacagaa gacatgagga aaaacaaaag gtttgaggaa atcaggcata tgactttata 1860 cttaacatca gatcttttct ataatatcct actactttgg ttttcctagc tccataccac 1920 acacctaaac ctgtattatg aattacatat tacaaagtca taaatgtgcc atatggatat 1980 acagtacatt ctagttggaa tcgtttactc tgctagaatt taggtgtgag attttttgtt 2040 tcccaggtat agcaggctta tgtttggtgg cattaaattg gtttctttaa aatgctttgg 2100 tggcactttt gtaaacagat tgcttctaga ttgttacaaa ccaagcctaa gacacatctg 2160 tgaatactta gatttgtagc ttaatcacat tctagacttg tgagttgaat gacaaagcag 2220 ttgaacaaaa attatggcat ttaagaattt aacatgtctt agctgtaaaa atgagaaagt 2280 gttggttggt tttaaaatct ggtaactcca tgatgaaaag aaatttattt tatacgtgtt 2340 atgtctctaa taaagtattc atttgataaa aaaaaaaaaa aa 2382 <210> SEQ ID NO 181 <211> LENGTH: 2377 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 181 atctttatgc aagacaagag tcagccatca gacactgaaa tatattatga tagattatga 60 agaattttct ctgtagaatt atattcttcc tggaacctgg tagagtagat tagactcaaa 120 ggctttttct tccttttctt actcctgttt tttccactca ctcttcccaa gagatttcct 180 aaagcttcaa gcttaataag cctaatagtg aaaaataact gaatttaatg gtataatgaa 240 gttcttcatt tccagacatc tttaattgat cttaaagctc atttgagtct ttgcccctga 300 acaaagacag acccattaaa atctaagaat tctaaatttt cacaactgtt tgagcttctt 360 ttcattttga aggatttgga atatatatgt tttcataaaa gtatcaagtg aaatatagtt 420 acatgggagc tcaatcatgt gcagattgca ttctgttatg ttgactcaat atttaattta 480 caactatcct tatttatatt gacctcaaga actccatttt atgcaatgca gaccactgag 540 atatagctaa cattctttca aataattttc cttttctttt ataattcctc tatagcaaat 600 ttttatgtat aactgattat acatatccat atttatattt cattgattcc aagacatcac 660 tttttcaatt taacatctct gaaattgtga catttcttgc aactgttggc acttcagatg 720 cagtgtttaa aattatgctt gaataaatat tacactaatc caactttacc taaatgttta 780 tgcatctagg caaattttgt tttcttataa agatttgaga gcccatttat gacaaaatat 840 gaaggcgaaa tttaaggaca actgagtcac gcacaactca acatggagcc taactgatta 900 tcagctcaga tcccgcatat cttgagttta caaaagctct ttcaggtccc catttatact 960 ttacgtgagt gcgaatgatt tcagcaaacc ctaacttaac taacaagaat gggtaggtat 1020 gtctacgttt cattaacaaa tttttattat ttttattcta ttatatgaga tccttttata 1080 ttatcatctc acttttaaac aaaattaact ggaaaaatat tacatggaac tgtcatagtt 1140 aggttttgca gcatcttaca tgtcttgtat caatggcagg agaaaaatat gataaaaaca 1200 atcagtgctg tgaaaaacaa ctttcttcta gagtcctctt actttttatt cttctttatc 1260 atttgtgggt ttttccccct tggctctcac tttaacttca agcttatgta acgactgtta 1320 taaaactgca tatttaaatt atttgaatta tatgaaataa ttgttcagct atctgggcag 1380 ctgttaatgt aaacctgaga gtaataacac tactctttta tctacctgga atacttttct 1440 gcataaaatt tatctttgta agctaactct attaatcagg tttcttctag cctctgcaac 1500 ctacttcagt tagaattgtc taatactgct ctattaatca ggtttctacc ctctacaacc 1560 tacttcagtt aaaattgtct aatacagcaa tatttaaaaa aaaaacactg caattgtcaa 1620 ggatggaaaa tgtgtgattt gtgtaaacaa tttttaccaa ctttacattt tcctacagat 1680 aaatgtgaaa ttttgataag aagtctacgc aatgacaagt acggtacata aattttatta 1740 agaatattga gtataaagta ctttaattct aaattataag aaaatataca tttgcacata 1800 ttaatataga aattcatttt gtgtatattt aacatagctt ttaaactatt ttacattagc 1860 tacttcatta tggtttcttg aacttctgaa aaaaattaga aatgtattaa acttatcagt 1920 aacataaaaa cttattttgt ttcacctaac gaatactgcg tttgtaaaaa taaatttaat 1980 atagaatata tttttaaatt aaatatttga atataaaata gctctaagaa agaagcaaat 2040 tatcactgaa catatttctt attatttctg gctttgaatt atacgtaact taaattgtct 2100 taaatgatac agaatattgg agaatatgat actttcacat aatatactat gaacctgttc 2160 atataactct gattgactac taacttctgt tttatgtatt tattaaagag ctgacactgt 2220 agtttgtggt gagatgttta tttttctaac agagcttata acagttagga caaggcattt 2280 aattaatgca tcattctgtt tagtagtagg tgttaatcaa tatgaaattc tctgttttaa 2340 aataaaaatg taaaaatcta aaaaaaaaaa aaaaaaa 2377 <210> SEQ ID NO 182 <211> LENGTH: 1370 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 182 tgtgagcatg gtattttgtc tcggaagaaa aaaatatggg tcaggcgcaa agtaagccca 60 ccccactggg aactatgtta aaaaaaaatt tcaagattta agggagatta cggtgttact 120 atgacaccag aaaaacttag aactttgtgt gaaatagact ggctaacatt agaggtgggt 180 tggctatcag aagaaagcct ggagaggtcc cttgtttcaa aggtatggca caaggtaacc 240 tgtaagccaa agcacccgga ccagtttcta tacatagaca gttacagctg gtttagaccc 300 cttccccctc tccccacagt agttaagaga acagcagcat aagcagctgg cagaggcaag 360 gaaagaccag cagagagaaa aaaaggccat ctataccaat tttaagttaa tttagactga 420 acaagggctt attaatagca aaggataatt gaaatcacaa acttataagg gtttcaacaa 480 aagtgaagtt tgctaaaagt taacagtgta acatgtatta tggtaacttc taatcttgtg 540 gccttagaca gtctagtcaa aacacataaa gaaagtttgc tttaaaaaaa caatggttat 600 cttcaaaaat aaaggggaga ggcagaattt atataaaaag agttatatga taaattcttg 660 tcctgaaata aattaactgg ttgtttaaag aaaagaatgt ttgtaataag tcaaaaagtt 720 aaaacatgtt taaaaaattg tctgcaaaag tcataaaaga aaaaatttta ttaaaaaaat 780 tttaagcaaa aaatgttgta taatttaaaa gtaataaggc ctcctgtgta ctattaagac 840 agatgcaaat tcctggttga aatggatcaa atattccatc tgcacattaa acaaaagcaa 900 ttgttatgct tgtgcacatg gcaggccaga ggccctgatt gtcccccttc cactaaggtg 960 gtcctctagt cgaccaggcg tggactgcat ggtagctctt ttccaggatt ctacagcctg 1020 gagtaataag tcatgccaag ctctctctgc tatatcccaa agtctctgcg ggtcagcccc 1080 caagggccat gcagcttctg tctcccaaca ctaagttcac ttcgtgtctc tcacggcaga 1140 gaggaaactt agtattcctt ggagacctga agggatgcag tgagcttaag aattttcaag 1200 agcttatcaa tcagtcagcc cttgttcatc cccgagtgga tgtgtggtgg tattgtggtg 1260 gacctttact gggcactctg ccaaataact agtgtggcac ttgtgcttta gtccatttgg 1320 ctatcccttt caccctggca tttcatcaac caaaaaaaaa aaaaaaaaaa 1370 <210> SEQ ID NO 183 <211> LENGTH: 2060 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 2003 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 183 gtttcagggg aggagacaag gtttcttgtt tgccgtatat gctcctgcag agaagaggaa 60 gtgaccgtgg aggccatctg gccctgtgtt ttgatatggc aaaattaatg aatgcaatca 120 gaagaccttt gagcaagaaa gtaccctgga acaacccaat ttggactgca agtattagtt 180 gggtcttcca ggtgcctctc acagcagcag tcatggcagc agtgactcta gccatgtcca 240 tgaccaactg ctgcataaca aatagccccg agactcagca gcttacaaca gggtccccag 300 cccacagact ggcactggtc catggcttgt taggaacctg actgcgcagc agaaggtgag 360 tgagcattac tgcctgagct ctgcctcctg tcagatcatc aggggcatta gattctcata 420 ggagcgtgaa ccctattgca aaccgcgcat gcgaaggatg tacgttgcgt gctccttatg 480 agaatctaac taatgcctga tgatttgagg tggggcagtt tcatccccaa accatctctc 540 tcccttcatg tccatggaaa aattgtcttc tacaaaacca gtccgtggtg ccaaaaaggt 600 tggagactgc tggtttacaa ccgcaatgaa cattcatcat cccacacagt gtcagagggt 660 cgggaacacg ggtgccctgc ctgtgtgctt ccggttccag atttctcagt gggttgtgat 720 caaggtatca gcggaggccg tattcatctg caagcttgac caggaataga agagccactt 780 catgggtggc tcactcagat gccagcaggt cagtgctggt ggctggcagg cagcctcagc 840 tcctcacctc atggatctct cctgagcaca gttttcctgt ccttacaacc tggtagctgg 900 cttctccaga gcaggtgact caggagagga caaggtgaga gcccagcacc ttatggtcta 960 gtctcagaag tcacacgcca tcatttctgc aatgtcattt tggggttcca ggtcagctgt 1020 atcactgtgg gaggtgagta tatagatgtc ctagaccatt caggctgcta tgacagaaca 1080 ccatgaactg agtggctcat gaacaacaga aatttcccac agttctgtag gctgggaaat 1140 ccaagatcaa ggtggcagca ggttcagcgt ctgctaagct cctgcttttc atggattgca 1200 tcttctcact gtgtcctcac gtgatggaca gagcaaatga gctctcaggc actagtccca 1260 gccatgagga ctctgctttc atgactcatc actccgcaaa ggcccacctc catcagaaga 1320 cagctgctaa ctgcagctgc catcctccaa gacgggagac acagaattgg gggacatata 1380 cattgagatc tgaaaggcct ggacagcaac aggtggggat cgtgggggca tcttggaggg 1440 tggctgccgc agtaacattt ctgacccatg ctttctgctt gcactcatct cctgcctttg 1500 atcttcatta tctcargcag tccccacaac gactgtatct aggagttcat tttaccctca 1560 ttttacagat gaaacgtctc agagggtaat gtgcttgccc agtgtctcac aaatgcaaag 1620 tcactgaggt aggatttcaa cctaggtcca atcatctctg cagcattagg ggttcaccat 1680 tgccatagac ttaactgtgt cccccaaaat ttgtatgttg aagccctacc agcctccccc 1740 ccccaatgtg ctgatgtttg gagaaagggc ctttgggagg taattaggtt tagatgagat 1800 catgagggtg ggactctcat aatggcatta atgccatcag gtgaagagat accagagacc 1860 ttgtgtcctc tctctctgca atgtgaggac acagtgagaa ggcagctgtc tgcaagctgg 1920 gaagagagta ctgaccagga acttaatcag agggcatctt gatcttggac ttcccagcct 1980 ccagaactct gaaaagttaa tgnctattat ttaagccacg cagtctatgg aattttgtta 2040 gagccaaccc caagcttact 2060 <210> SEQ ID NO 184 <211> LENGTH: 3079 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 184 ggcacaaagt tgggggccgc gaagatgagg ctgtccccgg cgcccctgaa gctgagccgg 60 actccggcac tgctggccct ggcgctgccc ctggccgcgg cgctggcctt ctccgacgag 120 accctggaca aagtgcccaa gtcagagggc tactgtagcc gtatcctgcg cgcccagggc 180 acgcggcgcg agggctacac cgagttcagc ctccgcgtgg agggcgaccc cgacttctac 240 aagccgggaa ccagctaccg cgtaacactt tcagctgctc ctccctccta cttcagagga 300 ttcacattaa ttgccctcag agagaacaga gagggtgata aggaagaaga ccatgctggg 360 accttccaga tcatagacga agaagaaact cagtttatga gcaattgccc tgttgcagtc 420 actgaaagca ctccacggag gaggacccgg atccaggtgt tttggatagc accaccagcg 480 ggaacaggct gcgtgattct gaaggccagc atcgtacaaa aacgcattat ttattttcaa 540 gatgagggct ctctgaccaa gaaactttgt gaacaagatt ccacatttga tggggtgact 600 gacaaaccca tcttagactg ctgtgcctgc ggaactgcca agtacagact cacattttat 660 gggaattggt ccgagaagac acacccaaag gattaccctc gtcgggccaa ccactggtct 720 gcgatcatcg gaggatccca ctccaagaat tatgtactgt gggaatatgg aggatatgcc 780 agcgaaggcg tcaaacaagt tgcagaattg ggctcacccg tgaaaatgga ggaagaaatt 840 cgacaacaga gtgatgaggt cctcaccgtc atcaaagcca aagcccaatg gccagcctgg 900 cagcctctca acgtgagagc agcaccttca gctgaatttt ccgtggacag aacgcgccat 960 ttaatgtcct tcctgaccat gatgggccct agtcccgact ggaacgtagg cttatctgca 1020 gaagatctgt gcaccaagga atgtggctgg gtccagaagg tggtgcaaga cctgattccc 1080 tgggacgctg gcaccgacag cggggtgacc tatgagtcac ccaacaaacc caccattccc 1140 caggagaaaa tccggcccct gaccagcctg gaccatcctc agagtccttt ctatgaccca 1200 gagggtgggt ccatcactca agtagccaga gttgtcatcg agagaatcgc acggaagggt 1260 gaacaatgca atattgtacc tgacaatgtc gatgatattg tagctgacct ggctccagaa 1320 gagaaagatg aagatgacac ccctgaaacc tgcatctact ccaactggtc cccatggtcc 1380 gcctgcagct cctccacctg tgacaaaggc aagaggatgc gacagcgcat gctgaaagca 1440 cagctggacc tcagcgtccc ctgccctgac acccaggact tccagccctg catgggccct 1500 ggctgcagtg acgaagacgg ctccacctgc accatgtccg agtggatcac ctggtcgccc 1560 tgcagcatct cctgcggcat gggcatgagg tcccgggaga ggtatgtgaa gcagttcccg 1620 gaggacggct ccgtgtgcac gctgcccact gaggaaatgg agaagtgcac ggtcaacgag 1680 gagtgctctc ccagcagctg cctgatgacc gagtggggcg agtgggacga gtgcagcgcc 1740 acctgcggca tgggcatgaa gaagcggcac cgcatgatca agatgaaccc cgcagatggc 1800 tccatgtgca aagccgagac atcacaggca gagaagtgca tgatgccaga gtgccacacc 1860 atcccatgct tgctgtcccc atggtccgag tggagtgact gcagcgtgac ctgcgggaag 1920 ggcatgcgaa cccgacagcg gatgctcaag tctctggcag aacttggaga ctgcaatgag 1980 gatctggagc aggtggagaa gtgcatgctc cctgaatgcc ccattgactg tgagctcacc 2040 gagtggtccc agtggtcgga atgtaacaag tcatgtggga aaggccacgt gattcgaacc 2100 cggatgatcc aaatggagcc tcagtttgga ggtgcaccct gcccagagac tgtgcagcga 2160 aaaaagtgcc gcatccgaaa atgccttcga aatccatcca tccaaaagcc acgctggagg 2220 gaggcccgag agagccggcg gagtgagcag ctgaaggaag agtctgaagg ggagcagttc 2280 ccaggttgta ggatgcgccc atggacggcc tggtcagaat gcaccaaact gtgcggaggt 2340 ggaattcagg aacgttacat gactgtaaag aagagattca aaagctccca gtttaccagc 2400 tgcaaagaca agaaggagat cagagcatgc aatgttcatc cttgttagca agggtacgag 2460 ttccccaggg ctgcactcta gattccagag tcaccaatgg ctggattatt tgcttgttta 2520 agacaattta aattgtgtac gctagttttc atttttgcag tgtggttcgc ccagtagtct 2580 tgtggatgcc agagacatcc tttctgaata cttcttgatg ggtacaggct gagtggggcg 2640 ccctcacctc cagccagcct cttcctgcag aggagtagtg tcagccacct tgtactaagc 2700 tgaaacatgt ccctctggag cttccacctg gccagggagg acggagactt tgacctactc 2760 cacatggaga ggcaaccatg tctggaagtg actatgcctg agtcccaggg tgcggcaggt 2820 aggaaacatt cacagatgaa gacagcagat tccccacatt ctcatctttg gcctgttcaa 2880 tgaaaccatt gtttgcccat ctcttcttag tggaacttta ggtctctttt caagtctcct 2940 cagtcatcaa tagttcctgg ggaaaaacag agctggtaga cttgaagagg agcattgatg 3000 ttgggtggct tttgttcttt cactgagaaa ttcggaatac atttgtctca cccctgatat 3060 tggttcctga tgccccagc 3079 <210> SEQ ID NO 185 <211> LENGTH: 3000 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 185 gtttcagggg aggagacaag gtttcttgtt tgccgtatat gctcctgcag agaagaggaa 60 gtgaccgtgg aggccatctg gccctgtgtt ttgatatggc aaaattaatg aatgcaatca 120 gaagaccttt gagcaagaaa gtaccctgga acaacccaat ttggactgca agtattagtt 180 gggtcttcca ggtgcctctc acagcagcag tcatggcagc agtgactcta gccatgtcca 240 tgaccaactg ctgcataaca aatagccccg agactcagca gcttacaaca gggtccccag 300 cccacagact ggcactggtc catggcttgt taggaacctg actgcgcagc agaaggtgag 360 tgagcattac tgcctgagct ctgcctcctg tcagatcatc aggggcatta gattctcata 420 ggagcgtgaa ccctattgca aaccgcgcat gcgaaggatg tacgttgcgt gctccttatg 480 agaatctaac taatgcctga tgatttgagg tggggcagtt tcatccccaa accatctctc 540 tcccttcatg tccatggaaa aattgtcttc tacaaaacca gtccgtggtg ccaaaaaggt 600 tggagactgc tggtttacaa ccgcaatgaa cattcatcat cccacacagt gtcagagggt 660 cgggaacacg ggtgccctgc ctgtgtgctt ccggttccag atttctcagt gggttgtgat 720 caaggtatca gcggaggccg tattcatctg caagcttgac caggaataga agagccactt 780 catgggtggc tcactcagat gccagcaggt cagtgctggt ggctggcagg cagcctcagc 840 tcctcacctc atggatctct cctgagcaca gttttcctgt ccttacaacc tggtagctgg 900 cttctccaga gcaggtgact caggagagga caaggtgaga gccacagcac cttatggtct 960 agtctcagaa gtcacacgcc atcatttctg caatgtcatt ttggggttcc aggtcagctg 1020 tatcactgtg ggaggtgagt atatagatgt cctagaccat tcaggctgct atgacagaac 1080 accatgaact gagtggctca tgaacaacag aaatttccca cagttctgta ggctgggaaa 1140 tccaagatca aggtggcagc aggttcagcg tctgctaagc tcctgctttt catggattgc 1200 atcttctcac tgtgtcctca cgtgatggac agagcaaatg agctctcagg cactagtccc 1260 agccatgagg actctgcttt catgactcat cactccgcaa aggcccacct ccatcagaag 1320 acagctgcta actgcagctg ccatcctcca agacgggaga cacagaattg ggggacatat 1380 acattgagat ctgaaaggcc tggacagcaa caggtgggga tcgtgggggc atcttggagg 1440 gtggctgccg cagtaacatt tctgacccat gctttctgct tgcactcatc tcctgccttt 1500 gatcttcatt atctcaggca gtccccacaa cgactgtatc taggagttca ttttaccctc 1560 attttacaga tgaaacgtct cagagggtaa tgtgcttgcc cagtgtctca caaatgcaaa 1620 gtcactgagg taggatttca acctaggtcc aatcatctct gcagcattag gggttcacca 1680 ttgccataga cttaactgtg tcccccaaaa tttgtatgtt gaagccctac cagcctcccc 1740 cccccaatgt gctgatgttt ggagaaaggg cctttgggag gtaattaggt ttagatgaga 1800 tcatgagggt gggactctca taatggcatt aatgccatca ggtgaagaga taccagagac 1860 cttgtgtcct ctctctctgc aatgtgagga cacagtgaga aggcagctgt ctgcaagctg 1920 ggaagagagt actgaccagg aacttaatca gagggcatct tgatcttgga cttcccagcc 1980 tccagaactc tgaaaagtta atgtctatta tttaagccac gcagtctatg gaattttgtt 2040 agagccaacc caagcttact aagataatca gtatgctgca ctttctataa atgtaatttt 2100 tacatttata aaaacaaaac aagagatttg ctgctctata acaactgtac ctacattgta 2160 gatggaataa caaatctaca tacagattta gtaatctcta tgtagatata gaacatagtg 2220 tatctaatag agacatagtg tctgtggtct gatgttaatt ttaggaatta gccgtcactg 2280 attgggcctt gtccaggtat tcttctccct tgtcctggct ctgtaaccta gttatccttg 2340 tctttgctaa cccataacca actattgtat caggactatt atgccactac agatgatgca 2400 gtttgggttt actgtttctc accatttaga caatacttca tcaaatatat ttctgtatga 2460 ctttagtgat atcagttttt gattcattcc tgcatagatc tgggcaaatt gtagacctta 2520 ggaggtgtat tcaccatcca gttctctgga actgcttatg acatttttct ctgagctttc 2580 ttgtcccaaa aggagccttc ctaaaatagt ctttaagtgc ctttaaaaag agaaagagaa 2640 attaagagaa aaaaaacccc aaactcattc ctttactctg atgtgacagt cctcccagga 2700 cactgcagtg gcctgagttt tgctgttaat ttcattcact tatgtttggg ctatgtaaat 2760 tctgcctaga gctggaatgt cattatgtaa agaaatattt tttgtttata ttctttaata 2820 gtaccagtaa tgtatatctt attcagcttc gagaatataa ttgggttgtt tataaaaacc 2880 acacatcatc aaactcacat tgtaacgatt atttcacttt tcaaaaaaaa tggcattaga 2940 aaaacttgaa tgatgttagt tatcttaaag aagtgtgtac tatgtttaaa aaaaaaaaaa 3000 <210> SEQ ID NO 186 <211> LENGTH: 807 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 186 Met Arg Leu Ser Pro Ala Pro Leu Lys Leu Ser Arg Thr Pro Ala Leu 1 5 10 15 Leu Ala Leu Ala Leu Pro Leu Ala Ala Ala Leu Ala Phe Ser Asp Glu 20 25 30 Thr Leu Asp Lys Val Pro Lys Ser Glu Gly Tyr Cys Ser Arg Ile Leu 35 40 45 Arg Ala Gln Gly Thr Arg Arg Glu Gly Tyr Thr Glu Phe Ser Leu Arg 50 55 60 Val Glu Gly Asp Pro Asp Phe Tyr Lys Pro Gly Thr Ser Tyr Arg Val 65 70 75 80 Thr Leu Ser Ala Ala Pro Pro Ser Tyr Phe Arg Gly Phe Thr Leu Ile 85 90 95 Ala Leu Arg Glu Asn Arg Glu Gly Asp Lys Glu Glu Asp His Ala Gly 100 105 110 Thr Phe Gln Ile Ile Asp Glu Glu Glu Thr Gln Phe Met Ser Asn Cys 115 120 125 Pro Val Ala Val Thr Glu Ser Thr Pro Arg Arg Arg Thr Arg Ile Gln 130 135 140 Val Phe Trp Ile Ala Pro Pro Ala Gly Thr Gly Cys Val Ile Leu Lys 145 150 155 160 Ala Ser Ile Val Gln Lys Arg Ile Ile Tyr Phe Gln Asp Glu Gly Ser 165 170 175 Leu Thr Lys Lys Leu Cys Glu Gln Asp Ser Thr Phe Asp Gly Val Thr 180 185 190 Asp Lys Pro Ile Leu Asp Cys Cys Ala Cys Gly Thr Ala Lys Tyr Arg 195 200 205 Leu Thr Phe Tyr Gly Asn Trp Ser Glu Lys Thr His Pro Lys Asp Tyr 210 215 220 Pro Arg Arg Ala Asn His Trp Ser Ala Ile Ile Gly Gly Ser His Ser 225 230 235 240 Lys Asn Tyr Val Leu Trp Glu Tyr Gly Gly Tyr Ala Ser Glu Gly Val 245 250 255 Lys Gln Val Ala Glu Leu Gly Ser Pro Val Lys Met Glu Glu Glu Ile 260 265 270 Arg Gln Gln Ser Asp Glu Val Leu Thr Val Ile Lys Ala Lys Ala Gln 275 280 285 Trp Pro Ala Trp Gln Pro Leu Asn Val Arg Ala Ala Pro Ser Ala Glu 290 295 300 Phe Ser Val Asp Arg Thr Arg His Leu Met Ser Phe Leu Thr Met Met 305 310 315 320 Gly Pro Ser Pro Asp Trp Asn Val Gly Leu Ser Ala Glu Asp Leu Cys 325 330 335 Thr Lys Glu Cys Gly Trp Val Gln Lys Val Val Gln Asp Leu Ile Pro 340 345 350 Trp Asp Ala Gly Thr Asp Ser Gly Val Thr Tyr Glu Ser Pro Asn Lys 355 360 365 Pro Thr Ile Pro Gln Glu Lys Ile Arg Pro Leu Thr Ser Leu Asp His 370 375 380 Pro Gln Ser Pro Phe Tyr Asp Pro Glu Gly Gly Ser Ile Thr Gln Val 385 390 395 400 Ala Arg Val Val Ile Glu Arg Ile Ala Arg Lys Gly Glu Gln Cys Asn 405 410 415 Ile Val Pro Asp Asn Val Asp Asp Ile Val Ala Asp Leu Ala Pro Glu 420 425 430 Glu Lys Asp Glu Asp Asp Thr Pro Glu Thr Cys Ile Tyr Ser Asn Trp 435 440 445 Ser Pro Trp Ser Ala Cys Ser Ser Ser Thr Cys Asp Lys Gly Lys Arg 450 455 460 Met Arg Gln Arg Met Leu Lys Ala Gln Leu Asp Leu Ser Val Pro Cys 465 470 475 480 Pro Asp Thr Gln Asp Phe Gln Pro Cys Met Gly Pro Gly Cys Ser Asp 485 490 495 Glu Asp Gly Ser Thr Cys Thr Met Ser Glu Trp Ile Thr Trp Ser Pro 500 505 510 Cys Ser Ile Ser Cys Gly Met Gly Met Arg Ser Arg Glu Arg Tyr Val 515 520 525 Lys Gln Phe Pro Glu Asp Gly Ser Val Cys Thr Leu Pro Thr Glu Glu 530 535 540 Met Glu Lys Cys Thr Val Asn Glu Glu Cys Ser Pro Ser Ser Cys Leu 545 550 555 560 Met Thr Glu Trp Gly Glu Trp Asp Glu Cys Ser Ala Thr Cys Gly Met 565 570 575 Gly Met Lys Lys Arg His Arg Met Ile Lys Met Asn Pro Ala Asp Gly 580 585 590 Ser Met Cys Lys Ala Glu Thr Ser Gln Ala Glu Lys Cys Met Met Pro 595 600 605 Glu Cys His Thr Ile Pro Cys Leu Leu Ser Pro Trp Ser Glu Trp Ser 610 615 620 Asp Cys Ser Val Thr Cys Gly Lys Gly Met Arg Thr Arg Gln Arg Met 625 630 635 640 Leu Lys Ser Leu Ala Glu Leu Gly Asp Cys Asn Glu Asp Leu Glu Gln 645 650 655 Val Glu Lys Cys Met Leu Pro Glu Cys Pro Ile Asp Cys Glu Leu Thr 660 665 670 Glu Trp Ser Gln Trp Ser Glu Cys Asn Lys Ser Cys Gly Lys Gly His 675 680 685 Val Ile Arg Thr Arg Met Ile Gln Met Glu Pro Gln Phe Gly Gly Ala 690 695 700 Pro Cys Pro Glu Thr Val Gln Arg Lys Lys Cys Arg Ile Arg Lys Cys 705 710 715 720 Leu Arg Asn Pro Ser Ile Gln Lys Pro Arg Trp Arg Glu Ala Arg Glu 725 730 735 Ser Arg Arg Ser Glu Gln Leu Lys Glu Glu Ser Glu Gly Glu Gln Phe 740 745 750 Pro Gly Cys Arg Met Arg Pro Trp Thr Ala Trp Ser Glu Cys Thr Lys 755 760 765 Leu Cys Gly Gly Gly Ile Gln Glu Arg Tyr Met Thr Val Lys Lys Arg 770 775 780 Phe Lys Ser Ser Gln Phe Thr Ser Cys Lys Asp Lys Lys Glu Ile Arg 785 790 795 800 Ala Cys Asn Val His Pro Cys 805 <210> SEQ ID NO 187 <211> LENGTH: 892 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 187 tttattgatg tttcaacagg cacttattca aataagttat atatttgaaa acagccatgg 60 taagcatcct tggcttctca cccattcctc atgtggcatg ctttctagac tttaaaatga 120 ggtaccctga atagcactaa gtgctctgta agctcaagga atctgtgcag tgctacaaag 180 cccacaggca gagaaagaac tcctcaagtg cttgtggtca gagactaggt tccatatgag 240 gcacacctat gatgaaggtc ttcacctcca gaaggtgaca ctgttcagag atcctcattt 300 cctggagagt gggagaaaat ccctcctttg ggaaatccct tttcccagca gcagagccca 360 cctcattgct tagtgatcat ttggaaggca ctgagagcct tcaggggctg acagcagaga 420 aatgaaaatg agtacagttc agatggtgga agaagcatgg cagtgacatc ttccatgctc 480 tttttctcag tgtctgcaac tccaaagatc aaggccataa cccaggagac catcaacgga 540 agattagttc tttgtcaagt gaatgaaatc caaaagcacg catgagacca atgaaagttt 600 ccgcctgttg taaaatctat tttcccccaa ggaaagtcct tgcacagaca ccagtgagtg 660 agttctaaaa gatacccttg gaattatcag actcagaaac ttttattttt tttttctgta 720 acagtctcac cagacttctc ataatgctct taatatattg cacttttcta atcaaagtgc 780 gagtttatga gggtaaagct ctactttcct actgcagcct tcagattctc atcattttgc 840 atctattttg tagccaataa aactccgcac tagcaaaaaa aaaaaaaaaa aa 892 <210> SEQ ID NO 188 <211> LENGTH: 1448 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1124 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 188 tgtgactcac atttctttta ctgtgacaca ataatgtgat cctaaaactg gcttatcctt 60 gagtgtttac aactcaaaca actttttgaa tgcagtagtt tttttttttt aaaaacaaac 120 ttttatgtca aatttttttt cttagaagta gtcttcatta ttataaattt gtacaccaaa 180 aggccatggg gaactttgtg caagtacctc atcgctgagc aaatggagct tgctatgttt 240 taatttcaga aaatttcctc atatacgtag tgtgtagaat caagtctttt aataattcat 300 tttttcttca taatatttac tcaaagttaa gcttaaaaat aagttttatc ttaaaatcat 360 atttgaagac agtaagacag taaactattt taggaagtca acccccattg cactctgtgg 420 cagttattct ggtaaaaata ggcaaaagtg acctgaatct acaatggtgt cccaaagtaa 480 ccaagtaaga gagattgtaa atgataaacc gagctttaaa ggataaagtg ttaataaaga 540 aaggaagctg ggcacatgtc aaaaagggag atcgaaatgt taggtaatca tttagaaagg 600 acagaaaata tttaaagtgg ctcataggta atgaatattt ctgacttaga tgtaaatcca 660 tctggaatct ttacatcctt tgccagctga aacaagaaag tgaagggaca atgatatttc 720 atggtcagtt tattttgtaa gagacagaag aaattatatc tatacattac cttgtagcag 780 cagtacctgg aagccccagc ccgtcacaga agtgtggagg ggggctcctg actagacaat 840 ttccctagcc cttgtgattt gaagcatgaa agttctggca ggttatgagc agcactaggg 900 ataaagtatg gttttatttt ggtgtaattt aggtttttca acaaagccct tgtctaaaat 960 aaaaggcatt attggaaata tttgaaaact agaaaatgat ggataaaagg gctgataaga 1020 aaatttctga ctgtcagtag aagtgagata agatcctcag aggaaacagt aagaagggat 1080 aatcattaag atagtaaaac aggcaaagca gaatcacatg tgcncacaca catacacatg 1140 taaacattgg aatgcataag ttttaatatt ttagcgctat cagtttctaa atgcattaat 1200 tactaactgc cctctcccaa gattcattta gttcaaacag tatccgtaaa ctaggaataa 1260 tgccacatgc attcaatggg atcttttaag tactcttcag tttgttccaa gaaatgtgcc 1320 tactgaaatc aaattaattt gtattcaatg tgtacttcaa gactgctaat tgtttcatct 1380 gaaagcctac aatgaatcat tgttcamcct tgaaaaataa aattttgtaa atcaaaaaaa 1440 aaaaaaaa 1448 <210> SEQ ID NO 189 <211> LENGTH: 460 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 189 ttttgggagc acggactgtc agttctctgg gaagtggtca gcgcatcctg cagggcttct 60 cctcctctgt cttttggaga accagggctc ttctcagggg ctctagggac tgccaggctg 120 tttcagccag gaaggccaaa atcaagagtg agatgtagaa agttgtaaaa tagaaaaagt 180 ggagttggtg aatcggttgt tctttcctca catttggatg attgtcataa ggtttttagc 240 atgttcctcc ttttcttcac cctccccttt tttcttctat taatcaagag aaacttcaaa 300 gttaatggga tggtcggatc tcacaggctg agaactcgtt cacctccaag catttcatga 360 aaaagctgct tcttattaat catacaaact ctcaccatga tgtgaagagt ttcacaaatc 420 cttcaaaata aaaagtaatg acttaaaaaa aaaaaaaaaa 460 <210> SEQ ID NO 190 <211> LENGTH: 481 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 190 aggtggtgga agaaactgtg gcacgaggtg actgaggtat ctgtgggagc taatcctgtc 60 caggtggaag taggagaatt tgatgatggt gcagaggaaa ccgaagagga ggtggtggcg 120 gaaaatccct gccagaacca ccactgcaaa cacggcaagg tgtgcgagct ggatgagaac 180 aacaccccca tgtgcgtgtg ccaggacccc accagctgcc cagcccccat tggcgagttt 240 gagaaggtgt gcagcaatga caacaagacc ttcgactctt cctgccactt ctttgccaca 300 aagtgcaccc tggagggcac caagaagggc cacaagctcc acctggacta catcgggcct 360 tgcaaataca tccccccttg cctggactct gagctgaccg aattccccct gcgcatgcgg 420 gactggctca agaacgtcct ggtcaccctg tatgagaggg atgaggacaa caaccttctg 480 a 481 <210> SEQ ID NO 191 <211> LENGTH: 489 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 312, 455 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 191 atataaatta gactaagtgt tttcaaataa atctaaatct tcagcatgat gtgttgtgta 60 taattggagt agatattaat taagtcccct gtataatgtt ttgtaatttt gcaaaacata 120 tcttgagttg tttaaacagt caaaatgttt gatattttat accagcttat gagctcaaag 180 tactacagca aagcctagcc tgcatatcat tcacccaaaa caaagtaata gcgcctcttt 240 tattattttg actgaatgtt ttatggaatt gaaagaaaca tacgttcttt tcaagacttc 300 ctcatgaatc tntcaattat aggaaaagtt attgtgataa aataggaaca gctgaaagat 360 tgattaatga actattgtta attcttccta ttttaatgaa tgacattgaa ctgaattttt 420 tgtctgttaa atgaacttga tagctaataa aaagncaact agccatcaaa aaaaaaaaaa 480 aaaaaaaaa 489 <210> SEQ ID NO 192 <211> LENGTH: 516 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 192 acttcaaagc cagctgaagg aaagaggaag tgctagagag agcccccttc agtgtgcttc 60 tgacttttac ggacttggct tgttagaagg ctgaaagatg atggcaggaa tgaaaatcca 120 gcttgtatgc atgctactcc tggctttcag ctcctggagt ctgtgctcag attcagaaga 180 ggaaatgaaa gcattagaag cagatttctt gaccaatatg catacatcaa agattagtaa 240 agcacatgtt ccctcttgga agatgactct gctaaatgtt tgcagtcttg taaataattt 300 gaacagccca gctgaggaaa caggagaagt tcatgaagag gagcttgttg caagaaggaa 360 cttcttactg ctttagatgg ctttagcttg gaagcaatgt tgacaatata ccagctccac 420 aaaatctgtc acagcagggc ttttcaacac tgggagttaa tccaggaaga tattcttgat 480 actggaaatg acaaaaatgg aaaggaagaa gtcata 516 <210> SEQ ID NO 193 <211> LENGTH: 1409 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 193 tgattctttt ccaaaacttt tagccatagg gtcttttata gacagggata gtaaaatgaa 60 aattgagaaa tataagatga aaaggaatgg taaaaatatc ttttaggggg cttttaattg 120 gtgatctgaa atcttgggag aagctgttct tttcaggcct gaggtgctct tgactgtcgc 180 ctgcgcactg tgtaccccga gcaacattct aagggtgtgc tttcgccttg gctaactcct 240 ttgacctcat tcttcatata gtagtctagg aaaaagttgc aggtaattta aactgtctag 300 tggtacatag taactgaatt tctattccta tgagaaatga gaattattta tttgccatca 360 acacatttta tactttgcat ctccaaattt attgcggcga gacttgtcca ttgtgaaagt 420 tagagaacat tatgtttgta tcatttcttt cataaaacct caagagcatt tttaagccct 480 tttcatcaga cccagtgaaa actaaggata gatgtttttt aactggaggt ctcctgataa 540 ggagaacaca atccaccatt gtcatttaag taataagaca ggaaattgac cttgacgctt 600 tcttgttaaa tagatttaac aggaacatct gcacatcttt tttccttgtg cactatttgt 660 ttaattgcag tggattaata cagcaagagt gccacattat aactaggcaa ttatccattc 720 ttcaagactt agttattgtc acactaattg atcgtttaag gcataagatg gtctagcatt 780 aggaacatgt gaagctaatc tgctcaaaaa gatcaacaaa ttaatattgt tgctgatatt 840 tgcataattg gctgcaatta tttaatgttt aattgggttg atcaaatgag attcagcaat 900 tcacaagtgc attaatataa acagaactgg ggcacttaaa atgataatga ttaacttata 960 ttgcatgttc tcttcctttc acttttttca gtgtctacat ttcagaccga gtttgtcagc 1020 ttttttgaaa acacatcagt agaaaccaag attttaaaat gaagtgtcaa gacgaaggca 1080 aaacctgagc agttcctaaa aagatttgct gttagaaatt ttctttgtgg cagtcattta 1140 ttaaggattc aactcgtgat acaccaaaag aagagttgac ttcagagatg tgttccatgc 1200 tctctagcac aggaatgaat aaatttataa cacctgcttt agcctttgtt ttcaaaagca 1260 caaaggaaaa gtgaaaggga aagagaaaca agtgactgag aagtcttgtt aaggaatcag 1320 gttttttcta cctggtaaac attctctatt cttttctcaa aagattgttg taagaaaaaa 1380 tgtaagmcaa aaaaaaaaaa aaaaaaaaa 1409 <210> SEQ ID NO 194 <211> LENGTH: 441 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 194 cagatttcgg tagccatctc cctccaaata tgtctctttc tgctttctta gtgcccatta 60 tttccccttc tcctttcttc tgtcactgcc atctccttct tggtcttccc attgttcttt 120 aactggccgt aatgtggaat tgatatttac attttgatac ggtttttttc ttggcctgtg 180 tacgggattg cctcatttcc tgctctgaat tttaaaatta gatattaaag ctgtcatatg 240 gtttcctcac aaaagtcaac aaagtccaaa caaaaatagt ttgccgtttt actttcatcc 300 attgaaaaag gaaattgtgc ctcttgcagc ctaggcaaag gacatttagt actatcgatt 360 ctttccaccc tcacgatgac ttgcggttct ctctgtagaa aagggatggc ctaagaaata 420 caactaaaaa aaaaaaaaaa a 441 <210> SEQ ID NO 195 <211> LENGTH: 707 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 195 cagaaaaata tttggaaaaa atataccact tcatagctaa gtcttacaga gaagaggatt 60 tgctaataaa acttaagttt tgaaaattaa gatgcaggta gagcttctga actaatgccc 120 acagctccaa ggaagacatg tcctatttag ttattcaaat acaagttgag ggcattgtga 180 ttaagcaaac aatatatttg ttagaacttt gtttttaaat tactgttcct tgacattact 240 tataaagagt ctctaacttt cgatttctaa aactatgtaa tacaaaagta tagtttcccc 300 atttgataaa aggccaatga tactgagtag gatatatgcg tatcatgcta cttcattcag 360 tgtgtctgtt tttaatacta ataaggcagt ttgacagaaa ttatttcttt gggactaagg 420 tgattatcat ttttttcccc ttcaaaattg tgctttaagt gctgataacc acaggcagat 480 tgcaaagaac tgataaggca acaaaagtag agaattttag gatcaaaggc atgtaactga 540 aaggtaacaa cagtacataa gcgacaactg gggaaggcag cagtgaaaca tgtttgtggg 600 gttaagtgag tcattgtaaa taaggaattt gcacatttat tttctgtcga cgcggccgcc 660 actgtgctgg atatctgcag aattccacca cactggacta gtggatc 707 <210> SEQ ID NO 196 <211> LENGTH: 552 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 61, 129, 189, 222, 241, 278, 324, 338, 363, 408, 415, 463, 483 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 196 tggccagcca gcctgatgtg gatggcttcc ttggggtggt gcttccctca agcccgaatt 60 ngtggacatc atcaatgcca aacaatgagc cccatccatt ttccctaccc ttcctgccaa 120 gccagggant aagcagccca gaagcccagt aactgccctt tccctgcata tgcttttgat 180 ggtgtcatnt gctccttcct gtggcctcat ccaaactgta tnttccttta ctgtttatat 240 nttcaccctg taatggttgg gaccaggcca atcccttntc cacttactat aatggttgga 300 actaaacgtc accaaggtgg cttntccttg gctgaganat ggaaggcgtg gtgggatttg 360 ctnctgggtt ccctaggccc tagtgagggc agaagagaaa ccatcctntc ccttnttaca 420 ccgtgaggcc aagatcccct cagaaggcag gagtgctgcc ctntcccatg gtgcccgtgc 480 ctntgtgctg tgtatgtgaa ccacccatgt gagggaataa acctggcact aggaaaaaaa 540 aaaaaaaaaa aa 552 <210> SEQ ID NO 197 <211> LENGTH: 449 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 56, 58, 76 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 197 ctccagagac aacttcgcgg tgtggtgaac tctctgagga aaaacacgtg cgtggnanca 60 agtgactgag acctanaaat ccaagcgttg gaggtcctga ggccagccta agtcgcttca 120 aaatggaacg aaggcgtttg cggggttcca ttcagagccg atacatcagc atgagtgtgt 180 ggacaagccc acggagactt gtggagctgg cagggcagag cctgctgaag gatgaggccc 240 tggccattgc ccgccctgga gttgctgccc agggagctct tcccgccact cttcatggca 300 gcctttgacg ggagacacag ccagaccctg aaggcaatgg tgcaggcctg gcccttcacc 360 tgcctccctc tgggagtgct gatgaaggga caacatcttc acctggagac cttcaaagct 420 gtgcttgatg gacttgatgt gctccttgc 449 <210> SEQ ID NO 198 <211> LENGTH: 606 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 198 tgagtttgcc cccttacccc catcccagtg aatatttgca attcctaaag acgtgttttg 60 attgtcacac ctgggtgggg aacatgctac tggcatctaa tgcatagagg gcagtaatgc 120 tgctaaacat ctttcaacgc acaggacaga gccccacaaa agagaattat ctagccccaa 180 atgtccataa cactgctgtt gagaaaacct accgcaggat cttactgggc ttcataggta 240 agcttgcctt tgttctggct tctgtagata tataaaataa agacactgcc cagtccctcc 300 ctcaacgtcc cgagccaggg ctcaaggcaa ttccaataac agtagaatga acactaaata 360 ttgatttcaa aatctcagca actagaagaa tgaccaacca tcctggttgg cctgggactg 420 tcctagtttt agcattgaaa gtttcaggtt ccaggaaagc cctcaggcct gggctgctgg 480 tcaccctagc agctgaggga ctcttcaata cagaattagt ctttgtgcac tggagatgaa 540 tatactttaa tttgtaacat gtgaaaacat ctataaacat ctactgaagc ctgttcttgt 600 ctgcac 606 <210> SEQ ID NO 199 <211> LENGTH: 369 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 29, 345 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 199 ggcaactttt tgcggattgt tcttgcttnc aggctttgcg ctgcaaatcc agtgctacca 60 gtgtgaagaa ttccagctga acaacgactg ctcctccccc gagttcattg tgaattgcac 120 ggtgaacgtt caagacatgt gtcagaaaga agtgatggag caaagtgccg ggatcatgta 180 ccgcaagtcc tgtgcatcat cagcggcctg tctcatcgcc tctgccgggt accagtcctt 240 ctgctcccca gggaaactga actcagtttg catcagctgc tgcaacaccc ctctttgtaa 300 cgggccaagg cccaagaaaa ggggaagttc tgcctcggcc ctcangccat ggctccgcac 360 caccatcct 369 <210> SEQ ID NO 200 <211> LENGTH: 55 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 200 Met Tyr Arg Asn Trp Ser Gly Cys Phe Gly Leu Gln Val Thr Leu Cys 1 5 10 15 His Thr Phe Glu Thr Arg Asp Leu Ser Arg Leu Ser Ser Asp Ser Gln 20 25 30 Pro Thr Ser Asn Val Ser Gln Ser Ile Ser His Lys Val Leu Ser Phe 35 40 45 Ser Gly Val Ile Val Thr Pro 50 55 <210> SEQ ID NO 201 <211> LENGTH: 67 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 201 Met Gln Leu Leu Ser Pro Asn Thr Lys Phe Thr Ser Cys Leu Ser Arg 1 5 10 15 Gln Arg Gly Asn Leu Val Phe Leu Gly Asp Leu Lys Gly Cys Ser Glu 20 25 30 Leu Lys Asn Phe Gln Glu Leu Ile Asn Gln Ser Ala Leu Val His Pro 35 40 45 Arg Val Asp Val Trp Trp Tyr Cys Gly Gly Pro Leu Leu Gly Thr Leu 50 55 60 Pro Asn Asn 65 <210> SEQ ID NO 202 <211> LENGTH: 73 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 202 Met Thr Pro Glu Lys Leu Arg Thr Leu Cys Glu Ile Asp Trp Leu Thr 1 5 10 15 Leu Glu Val Gly Trp Leu Ser Glu Glu Ser Leu Glu Arg Ser Leu Val 20 25 30 Ser Lys Val Trp His Lys Val Thr Cys Lys Pro Lys His Pro Asp Gln 35 40 45 Phe Leu Tyr Ile Asp Ser Tyr Ser Trp Phe Arg Pro Leu Pro Pro Leu 50 55 60 Pro Thr Val Val Lys Arg Thr Ala Ala 65 70 <210> SEQ ID NO 203 <211> LENGTH: 2008 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 203 ctccagagac aacttcgcgg tgtggtgaac tctctgagga aaaacacgtg cgtggtaaca 60 agtgactgag acctagaaat ccaagcgttg gaggtcctga ggccagccta agtcgcttca 120 aaatggaacg aaggcgtttg cggggttcca ttcagagccg atacatcagc atgagtgtgt 180 ggacaagccc acggagactt gtggagctgg cagggcagag cctgctgaag gatgaggccc 240 tggccattgc ccgccctgga gttgctgccc agggagctct tcccgccact cttcatggca 300 gcctttgacg ggagacacag ccagaccctg aaggcaatgg tgcaggcctg gcccttcacc 360 tgcctccctc tgggagtgct gatgaaggga caacatcttc acctggagac cttcaaagct 420 gtgcttgatg gacttgatgt gctccttgcc caggaggttc gccccaggag gtggaaactt 480 caagtgctgg atttacggaa gaactctcat caggacttct ggactgtatg gtctggaaac 540 agggccagtc tgtactcatt tccagagcca gaagcagctc agcccatgac aaagaagcga 600 aaagtagatg gtttgagcac agaggcagag cagcccttca ttccagtaga ggtgctcgta 660 gacctgttcc tcaaggaagg tgcctgtgat gaattgttct cctacctcat tgagaaagtg 720 aagcgaaaga aaaatgtact acgcctgtgc tgtaagaagc tgaagatttt tgcaatgccc 780 atgcaggata tcaagatgat cctgaaaatg gtgcagctgg actctattga agatttggaa 840 gtgacttgta cctggaagct acccaccttg gcgaaatttt ctccttacct gggccagatg 900 attaatctgc gtagactcct cctctcccac atccatgcat cttcctacat ttccccggag 960 aaggaagagc agtatatcgc ccagttcacc tctcagttcc tcagtctgca gtgcctgcag 1020 gctctctatg tggactcttt atttttcctt agaggccgcc tggatcagtt gctcaggcac 1080 gtgatgaacc ccttggaaac cctctcaata actaactgcc ggctttcgga aggggatgtg 1140 atgcatctgt cccagagtcc cagcgtcagt cagctaagtg tcctgagtct aagtggggtc 1200 atgctgaccg atgtaagtcc cgagcccctc caagctctgc tggagagagc ctctgccacc 1260 ctccaggacc tggtctttga tgagtgtggg atcacggatg atcagctcct tgccctcctg 1320 ccttccctga gccactgctc ccagcttaca accttaagct tctacgggaa ttccatctcc 1380 atatctgcct tgcagagtct cctgcagcac ctcatcgggc tgagcaatct gacccacgtg 1440 ctgtatcctg tccccctgga gagttatgag gacatccatg gtaccctcca cctggagagg 1500 cttgcctatc tgcatgccag gctcagggag ttgctgtgtg agttggggcg gcccagcatg 1560 gtctggctta gtgccaaccc ctgtcctcac tgtggggaca gaaccttcta tgacccggag 1620 cccatcctgt gcccctgttt catgcctaac tagctgggtg cacatatcaa atgcttcatt 1680 ctgcatactt ggacactaaa gccaggatgt gcatgcatct tgaagcaaca aagcagccac 1740 agtttcagac aaatgttcag tgtgagtgag gaaaacatgt tcagtgagga aaaaacattc 1800 agacaaatgt tcagtgagga aaaaaagggg aagttgggga taggcagatg ttgacttgag 1860 gagttaatgt gatctttggg gagatacatc ttatagagtt agaaatagaa tctgaatttc 1920 taaagggaga ttctggcttg ggaagtacat gtaggagtta atccctgtgt agactgttgt 1980 aaagaaactg ttgaaaaaaa aaaaaaaa 2008 <210> SEQ ID NO 204 <211> LENGTH: 923 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 204 tgagtttgcc cccttacccc catcccagtg aatatttgca attcctaaag acgtgttttg 60 attgtcacac ctgggtgggg aacatgctac tggcatctaa tgcatagagg gcagtaatgc 120 tgctaaacat ctttcaacgc acaggacaga gccccacaaa agagaattat ctagccccaa 180 atgtccataa cactgctgtt gagaaaacct accgcaggat cttactgggc ttcataggta 240 agcttgcctt tgttctggct tctgtagata tataaaataa agacactgcc cagtccctcc 300 ctcaacgtcc cgagccaggg ctcaaggcaa ttccaataac agtagaatga acactaaata 360 ttgatttcaa aatctcagca actagaagaa tgaccaacca tcctggttgg cctgggactg 420 tcctagtttt agcattgaaa gtttcaggtt ccaggaaagc cctcaggcct gggctgctgg 480 tcaccctagc agctgaggga ctcttcaata cagaattagt ctttgtgcac tggagatgaa 540 tatactttaa tttgtaacat gtgaaaacat ctataaacat ctactgaagc ctgttctgtc 600 tgcaccgaca ttttcattga gtacggattc ttcctaccag atacagctgc tctacaactt 660 tcgagggctg gtataaaact agcttttacc tatttttaaa aattacatga atagtaaaaa 720 cttggattaa cccagtattc gggtattttc aatttccttg ggagcttaga ggacggacaa 780 ataaaaagat tatttcaaca tcaaatatat gctattgttt acatatgaag ataaccacat 840 atatgtataa attcaccgtt actttttagc aatactataa aatccaacag aaaaaaatag 900 catttactaa aaaaaaaaaa aaa 923 <210> SEQ ID NO 205 <211> LENGTH: 1619 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 205 ggcaactttt tgcggattgt tcttgcttcc aggctttgcg ctgcaaatcc agtgctacca 60 gtgtgaagaa ttccagctga acaacgactg ctcctccccc gagttcattg tgaattgcac 120 ggtgaacgtt caagacatgt gtcagaaaga agtgatggag caaagtgccg ggatcatgta 180 ccgcaagtcc tgtgcatcat cagcggcctg tctcatcgcc tctgccgggt accagtcctt 240 ctgctcccca gggaaactga actcagtttg catcagctgc tgcaacaccc ctctttgtaa 300 cgggccaagg cccaagaaaa ggggaagttc tgcctcggcc ctcaggccag ggctccgcac 360 caccatcctg ttcctcaaat tagccctctt ctcggcacac tgctgaagct gaaggagatg 420 ccaccccctc ctgcattgtt cttccagccc tcgcccccaa ccccccacct ccctgagtga 480 gtttcttctg ggtgtccttt tattctgggt agggagcggg agtccgtgtt ctcttttgtt 540 cctgtgcaaa taatgaaaga gctcggtaaa gcattctgaa taaattcagc ctgactgaat 600 tttcagtatg tacttgaagg aaggaggtgg agtgaaagtt cacccccatg tctgtgtaac 660 cggagtcaag gccaggctgg cagagtcagt ccttagaagt cactgaggtg ggcatctgcc 720 ttttgtaaag cctccagtgt ccattccatc cctgatgggg gcatagtttg agactgcaga 780 gtgagagtga cgttttctta gggctggagg gccagttccc actcaaggct ccctcgcttg 840 acattcaaac ttcatgctcc tgaaaaccat tctctgcagc agaattggct ggtttcgcgc 900 ctgagttggg ctctagtgac tcgagactca atgactggga cttagactgg ggctcggcct 960 cgctctgaaa agtgcttaag aaaatcttct cagttctcct tgcagaggac tggcgccggg 1020 acgcgaagag caacgggcgc tgcacaaagc gggcgctgtc ggtggtggag tgcgcatgta 1080 cgcgcaggcg cttctcgtgg ttggcgtgct gcagcgacag gcggcagcac agcaccttgc 1140 acgaacaccc gccgaaactg ctgcgaggac accgtgtaca ggagcgggtt gatgaccgag 1200 ctgaggtaga aaaacgtctc cgagaagggg aggaggatca tgtacgcccg gaagtaggac 1260 ctcgtccagt cgtgcttggg tttggccgca gccatgatcc tccgaatctg gttgggcatc 1320 cagcatacgg ccaatgtcac aacaatcagc cctgggcaga cacgagcagg agggagagac 1380 agagaaaaga aaaacacagc atgagaacac agtaaatgaa taaaaccata aaatatttag 1440 cccctctgtt ctgtgcttac tggccaggaa atggtaccaa tttttcagtg ttggacttga 1500 cagcttcttt tgccacaagc aagagagaat ttaacactgt ttcaaacccg ggggagttgg 1560 ctgtgttaaa gaaagaccat taaatgcttt agacagtgta aaaaaaaaaa aaaaaaaaa 1619 <210> SEQ ID NO 206 <211> LENGTH: 2364 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 206 atgcagcatc accaccatca ccacttctcc gacgagaccc tggacaaagt gcccaagtca 60 gagggctact gtagccgtat cctgcgcgcc cagggcacgc ggcgcgaggg ctacaccgag 120 ttcagcctcc gcgtggaggg cgaccccgac ttctacaagc cgggaaccag ctaccgcgta 180 acactttcag ctgctcctcc ctcctacttc agaggattca cattaattgc cctcagagag 240 aacagagagg gtgataagga agaagaccat gctgggacct tccagatcat agacgaagaa 300 gaaactcagt ttatgagcaa ttgccctgtt gcagtcactg aaagcactcc acggaggagg 360 acccggatcc aggtgttttg gatagcacca ccagcgggaa caggctgcgt gattctgaag 420 gccagcatcg tacaaaaacg cattatttat tttcaagatg agggctctct gaccaagaaa 480 ctttgtgaac aagattccac atttgatggg gtgactgaca aacccatctt agactgctgt 540 gcctgcggaa ctgccaagta cagactcaca ttttatggga attggtccga gaagacacac 600 ccaaaggatt accctcgtcg ggccaaccac tggtctgcga tcatcggagg atcccactcc 660 aagaattatg tactgtggga atatggagga tatgccagcg aaggcgtcaa acaagttgca 720 gaattgggct cacccgtgaa aatggaggaa gaaattcgac aacagagtga tgaggtcctc 780 accgtcatca aagccaaagc ccagtggcca gcctggcagc ctctcaacgt gagagcagca 840 ccttcagctg aattttccgt ggacagaacg cgccatttaa tgtccttcct gaccatgatg 900 ggccctagtc ccgactggaa cgtaggctta tctgcagaag atctgtgcac caaggaatgt 960 ggctgggtcc agaaggtggt gcaagacctg attccctggg acgctggcac cgacagcggg 1020 gtgacctatg agtcacccaa caaacccacc attccccagg agaaaatccg gcccctgacc 1080 agcctggacc atcctcagag tcctttctat gacccagagg gtgggtccat cactcaagta 1140 gccagagttg tcatcgagag aatcgcacgg aagggtgaac aatgcaatat tgtacctgac 1200 aatgtcgatg atattgtagc tgacctggct ccagaagaga aagatgaaga tgacacccct 1260 gaaacctgca tctactccaa ctggtcccca tggtccgcct gcagctcctc cacctgtgac 1320 aaaggcaaga ggatgcgaca gcgcatgctg aaagcacagc tggacctcag cgtcccctgc 1380 cctgacaccc aggacttcca gccctgcatg ggccctggct gcagtgacga agacggctcc 1440 acctgcacca tgtccgagtg gatcacctgg tcgccctgca gcatctcctg cggcatgggc 1500 atgaggtccc gggagaggta tgtgaagcag ttcccggagg acggctccgt gtgcacgctg 1560 cccactgagg aaacggagaa gtgcacggtc aacgaggagt gctctcccag cagctgcctg 1620 atgaccgagt ggggcgagtg ggacgagtgc agcgccacct gcggcatggg catgaagaag 1680 cggcaccgca tgatcaagat gaaccccgca gatggctcca tgtgcaaagc cgagacatca 1740 caggcagaga agtgcatgat gccagagtgc cacaccatcc catgcttgct gtccccatgg 1800 tccgagtgga gtgactgcag cgtgacctgc gggaagggca tgcgaacccg acagcggatg 1860 ctcaagtctc tggcagaact tggagactgc aatgaggatc tggagcaggt ggagaagtgc 1920 atgctccctg aatgccccat tgactgtgag ctcaccgagt ggtcccagtg gtcggaatgt 1980 aacaagtcat gtgggaaagg ccacgtgatt cgaacccgga tgatccaaat ggagcctcag 2040 tttggaggtg caccctgccc agagactgtg cagcgaaaaa agtgccgcat ccgaaaatgc 2100 cttcgaaatc catccatcca aaagctacgc tggagggagg cccgagagag ccggcggagt 2160 gagcagctga aggaagagtc tgaaggggag cagttcccag gttgtaggat gcgcccatgg 2220 acggcctggt cagaatgcac caaactgtgc ggaggtggaa ttcaggaacg ttacatgact 2280 gtaaagaaga gattcaaaag ctcccagttt accagctgca aagacaagaa ggagatcaga 2340 gcatgcaatg ttcatccttg ttag 2364 <210> SEQ ID NO 207 <211> LENGTH: 787 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 207 Met Gln His His His His His His Phe Ser Asp Glu Thr Leu Asp Lys 1 5 10 15 Val Pro Lys Ser Glu Gly Tyr Cys Ser Arg Ile Leu Arg Ala Gln Gly 20 25 30 Thr Arg Arg Glu Gly Tyr Thr Glu Phe Ser Leu Arg Val Glu Gly Asp 35 40 45 Pro Asp Phe Tyr Lys Pro Gly Thr Ser Tyr Arg Val Thr Leu Ser Ala 50 55 60 Ala Pro Pro Ser Tyr Phe Arg Gly Phe Thr Leu Ile Ala Leu Arg Glu 65 70 75 80 Asn Arg Glu Gly Asp Lys Glu Glu Asp His Ala Gly Thr Phe Gln Ile 85 90 95 Ile Asp Glu Glu Glu Thr Gln Phe Met Ser Asn Cys Pro Val Ala Val 100 105 110 Thr Glu Ser Thr Pro Arg Arg Arg Thr Arg Ile Gln Val Phe Trp Ile 115 120 125 Ala Pro Pro Ala Gly Thr Gly Cys Val Ile Leu Lys Ala Ser Ile Val 130 135 140 Gln Lys Arg Ile Ile Tyr Phe Gln Asp Glu Gly Ser Leu Thr Lys Lys 145 150 155 160 Leu Cys Glu Gln Asp Ser Thr Phe Asp Gly Val Thr Asp Lys Pro Ile 165 170 175 Leu Asp Cys Cys Ala Cys Gly Thr Ala Lys Tyr Arg Leu Thr Phe Tyr 180 185 190 Gly Asn Trp Ser Glu Lys Thr His Pro Lys Asp Tyr Pro Arg Arg Ala 195 200 205 Asn His Trp Ser Ala Ile Ile Gly Gly Ser His Ser Lys Asn Tyr Val 210 215 220 Leu Trp Glu Tyr Gly Gly Tyr Ala Ser Glu Gly Val Lys Gln Val Ala 225 230 235 240 Glu Leu Gly Ser Pro Val Lys Met Glu Glu Glu Ile Arg Gln Gln Ser 245 250 255 Asp Glu Val Leu Thr Val Ile Lys Ala Lys Ala Gln Trp Pro Ala Trp 260 265 270 Gln Pro Leu Asn Val Arg Ala Ala Pro Ser Ala Glu Phe Ser Val Asp 275 280 285 Arg Thr Arg His Leu Met Ser Phe Leu Thr Met Met Gly Pro Ser Pro 290 295 300 Asp Trp Asn Val Gly Leu Ser Ala Glu Asp Leu Cys Thr Lys Glu Cys 305 310 315 320 Gly Trp Val Gln Lys Val Val Gln Asp Leu Ile Pro Trp Asp Ala Gly 325 330 335 Thr Asp Ser Gly Val Thr Tyr Glu Ser Pro Asn Lys Pro Thr Ile Pro 340 345 350 Gln Glu Lys Ile Arg Pro Leu Thr Ser Leu Asp His Pro Gln Ser Pro 355 360 365 Phe Tyr Asp Pro Glu Gly Gly Ser Ile Thr Gln Val Ala Arg Val Val 370 375 380 Ile Glu Arg Ile Ala Arg Lys Gly Glu Gln Cys Asn Ile Val Pro Asp 385 390 395 400 Asn Val Asp Asp Ile Val Ala Asp Leu Ala Pro Glu Glu Lys Asp Glu 405 410 415 Asp Asp Thr Pro Glu Thr Cys Ile Tyr Ser Asn Trp Ser Pro Trp Ser 420 425 430 Ala Cys Ser Ser Ser Thr Cys Asp Lys Gly Lys Arg Met Arg Gln Arg 435 440 445 Met Leu Lys Ala Gln Leu Asp Leu Ser Val Pro Cys Pro Asp Thr Gln 450 455 460 Asp Phe Gln Pro Cys Met Gly Pro Gly Cys Ser Asp Glu Asp Gly Ser 465 470 475 480 Thr Cys Thr Met Ser Glu Trp Ile Thr Trp Ser Pro Cys Ser Ile Ser 485 490 495 Cys Gly Met Gly Met Arg Ser Arg Glu Arg Tyr Val Lys Gln Phe Pro 500 505 510 Glu Asp Gly Ser Val Cys Thr Leu Pro Thr Glu Glu Thr Glu Lys Cys 515 520 525 Thr Val Asn Glu Glu Cys Ser Pro Ser Ser Cys Leu Met Thr Glu Trp 530 535 540 Gly Glu Trp Asp Glu Cys Ser Ala Thr Cys Gly Met Gly Met Lys Lys 545 550 555 560 Arg His Arg Met Ile Lys Met Asn Pro Ala Asp Gly Ser Met Cys Lys 565 570 575 Ala Glu Thr Ser Gln Ala Glu Lys Cys Met Met Pro Glu Cys His Thr 580 585 590 Ile Pro Cys Leu Leu Ser Pro Trp Ser Glu Trp Ser Asp Cys Ser Val 595 600 605 Thr Cys Gly Lys Gly Met Arg Thr Arg Gln Arg Met Leu Lys Ser Leu 610 615 620 Ala Glu Leu Gly Asp Cys Asn Glu Asp Leu Glu Gln Val Glu Lys Cys 625 630 635 640 Met Leu Pro Glu Cys Pro Ile Asp Cys Glu Leu Thr Glu Trp Ser Gln 645 650 655 Trp Ser Glu Cys Asn Lys Ser Cys Gly Lys Gly His Val Ile Arg Thr 660 665 670 Arg Met Ile Gln Met Glu Pro Gln Phe Gly Gly Ala Pro Cys Pro Glu 675 680 685 Thr Val Gln Arg Lys Lys Cys Arg Ile Arg Lys Cys Leu Arg Asn Pro 690 695 700 Ser Ile Gln Lys Leu Arg Trp Arg Glu Ala Arg Glu Ser Arg Arg Ser 705 710 715 720 Glu Gln Leu Lys Glu Glu Ser Glu Gly Glu Gln Phe Pro Gly Cys Arg 725 730 735 Met Arg Pro Trp Thr Ala Trp Ser Glu Cys Thr Lys Leu Cys Gly Gly 740 745 750 Gly Ile Gln Glu Arg Tyr Met Thr Val Lys Lys Arg Phe Lys Ser Ser 755 760 765 Gln Phe Thr Ser Cys Lys Asp Lys Lys Glu Ile Arg Ala Cys Asn Val 770 775 780 His Pro Cys 785 <210> SEQ ID NO 208 <211> LENGTH: 1362 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 208 atggcttcac ccagcctccc gggcagtgac tgctcccaaa tcattgatca cagtcatgtc 60 cccgagtttg aggtggccac ctggatcaaa atcaccctta ttctggtgta cctgatcatc 120 ttcgtgatgg gccttctggg gaacagcgcc accattcggg tcacccaggt gctgcagaag 180 aaaggatact tgcagaagga ggtgacagac cacatggtga gtttggcttg ctcggacatc 240 ttggtgttcc tcatcggcat gcccatggag ttctacagca tcatctggaa tcccctgacc 300 acgtccagct acaccctgtc ctgcaagctg cacactttcc tcttcgaggc ctgcagctac 360 gctacgctgc tgcacgtgct gacactcagc tttgagcgct acatcgccat ctgtcacccc 420 ttcaggtaca aggctgtgtc gggaccttgc caggtgaagc tgctgattgg cttcgtctgg 480 gtcacctccg ccctggtggc actgcccttg ctgtttgcca tgggtactga gtaccccctg 540 gtgaacgtgc ccagccaccg gggtctcact tgcaaccgct ccagcacccg ccaccacgag 600 cagcccgaga cctccaatat gtccatctgt accaacctct ccagccgctg gaccgtgttc 660 cagtccagca tcttcggcgc cttcgtggtc tacctcgtgg tcctgctctc cgtagccttc 720 atgtgctgga acatgatgca ggtgctcatg aaaagccaga agggctcgct ggccgggggc 780 acgcggcctc cgcagctgag gaagtccgag agcgaagaga gcaggaccgc caggaggcag 840 accatcatct tcctgaggct gattgttgtg acattggccg tatgctggat gcccaaccag 900 attcggagga tcatggctgc ggccaaaccc aagcacgact ggacgaggtc ctacttccgg 960 gcgtacatga tcctcctccc cttctcggag acgtttttct acctcagctc ggtcatcaac 1020 ccgctcctgt acacggtgtc ctcgcagcag tttcggcggg tgttcgtgca ggtgctgtgc 1080 tgccgcctgt cgctgcagca cgccaaccac gagaagcgcc tgcgcgtaca tgcgcactcc 1140 accaccgaca gcgcccgctt tgtgcagcgc ccgttgctct tcgcgtcccg gcgccagtcc 1200 tctgcaagga gaactgagaa gattttctta agcacttttc agagcgaggc cgagccccag 1260 tctaagtccc agtcattgag tctcgagtca ctagagccca actcaggcgc gaaaccagcc 1320 aattctgctg cagagaatgg ttttcaggag catgaagttt ga 1362 <210> SEQ ID NO 209 <211> LENGTH: 453 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 209 Met Ala Ser Pro Ser Leu Pro Gly Ser Asp Cys Ser Gln Ile Ile Asp 1 5 10 15 His Ser His Val Pro Glu Phe Glu Val Ala Thr Trp Ile Lys Ile Thr 20 25 30 Leu Ile Leu Val Tyr Leu Ile Ile Phe Val Met Gly Leu Leu Gly Asn 35 40 45 Ser Ala Thr Ile Arg Val Thr Gln Val Leu Gln Lys Lys Gly Tyr Leu 50 55 60 Gln Lys Glu Val Thr Asp His Met Val Ser Leu Ala Cys Ser Asp Ile 65 70 75 80 Leu Val Phe Leu Ile Gly Met Pro Met Glu Phe Tyr Ser Ile Ile Trp 85 90 95 Asn Pro Leu Thr Thr Ser Ser Tyr Thr Leu Ser Cys Lys Leu His Thr 100 105 110 Phe Leu Phe Glu Ala Cys Ser Tyr Ala Thr Leu Leu His Val Leu Thr 115 120 125 Leu Ser Phe Glu Arg Tyr Ile Ala Ile Cys His Pro Phe Arg Tyr Lys 130 135 140 Ala Val Ser Gly Pro Cys Gln Val Lys Leu Leu Ile Gly Phe Val Trp 145 150 155 160 Val Thr Ser Ala Leu Val Ala Leu Pro Leu Leu Phe Ala Met Gly Thr 165 170 175 Glu Tyr Pro Leu Val Asn Val Pro Ser His Arg Gly Leu Thr Cys Asn 180 185 190 Arg Ser Ser Thr Arg His His Glu Gln Pro Glu Thr Ser Asn Met Ser 195 200 205 Ile Cys Thr Asn Leu Ser Ser Arg Trp Thr Val Phe Gln Ser Ser Ile 210 215 220 Phe Gly Ala Phe Val Val Tyr Leu Val Val Leu Leu Ser Val Ala Phe 225 230 235 240 Met Cys Trp Asn Met Met Gln Val Leu Met Lys Ser Gln Lys Gly Ser 245 250 255 Leu Ala Gly Gly Thr Arg Pro Pro Gln Leu Arg Lys Ser Glu Ser Glu 260 265 270 Glu Ser Arg Thr Ala Arg Arg Gln Thr Ile Ile Phe Leu Arg Leu Ile 275 280 285 Val Val Thr Leu Ala Val Cys Trp Met Pro Asn Gln Ile Arg Arg Ile 290 295 300 Met Ala Ala Ala Lys Pro Lys His Asp Trp Thr Arg Ser Tyr Phe Arg 305 310 315 320 Ala Tyr Met Ile Leu Leu Pro Phe Ser Glu Thr Phe Phe Tyr Leu Ser 325 330 335 Ser Val Ile Asn Pro Leu Leu Tyr Thr Val Ser Ser Gln Gln Phe Arg 340 345 350 Arg Val Phe Val Gln Val Leu Cys Cys Arg Leu Ser Leu Gln His Ala 355 360 365 Asn His Glu Lys Arg Leu Arg Val His Ala His Ser Thr Thr Asp Ser 370 375 380 Ala Arg Phe Val Gln Arg Pro Leu Leu Phe Ala Ser Arg Arg Gln Ser 385 390 395 400 Ser Ala Arg Arg Thr Glu Lys Ile Phe Leu Ser Thr Phe Gln Ser Glu 405 410 415 Ala Glu Pro Gln Ser Lys Ser Gln Ser Leu Ser Leu Glu Ser Leu Glu 420 425 430 Pro Asn Ser Gly Ala Lys Pro Ala Asn Ser Ala Ala Glu Asn Gly Phe 435 440 445 Gln Glu His Glu Val 450 <210> SEQ ID NO 210 <211> LENGTH: 625 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 607 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 210 agttctcctt gcagaggact ggcgccggga cgcgaagagc aacgggcgct gcacaaagcg 60 ggcgctgtcg gtggtggagt gcgcatgtac gcgcaggcgc ttctcgtggt tggcgtgctg 120 cagcgacagg cggcagcaca gcacctgcac gaacacccgc cgaaactgct gcgaggacac 180 cgtgtacagg agcgggttga tgaccgagct gaggtagaaa aacgtctccg agaaggggag 240 gaggatcatg tacgcccgga agtaggacct cgtccagtcg tgcttgggtt tggccgcagc 300 catgatcctc cgaatctggt tgggcatcca gcatacggcc aatgtcacaa caatcagccc 360 tgggcagaca cgagcaggag ggagagacag agaaaagaaa aacacagcat gagaacacag 420 taaatgaata aaaccataaa atatttagcc cctctgttct gtgcttactg gccaggaaat 480 ggtaccaatt tttcagtgtt ggacttgaca gcttcttttg ccacaagcaa gagagaattt 540 aacactgttt caaacccggg ggagttggct gtgttaaaga aagaccatta aatgctttag 600 acagtgnaaa aaaaaaaaaa aaaaa 625 <210> SEQ ID NO 211 <211> LENGTH: 1619 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 211 ggcaactttt tgcggattgt tcttgcttcc aggctttgcg ctgcaaatcc agtgctacca 60 gtgtgaagaa ttccagctga acaacgactg ctcctccccc gagttcattg tgaattgcac 120 ggtgaacgtt caagacatgt gtcagaaaga agtgatggag caaagtgccg ggatcatgta 180 ccgcaagtcc tgtgcatcat cagcggcctg tctcatcgcc tctgccgggt accagtcctt 240 ctgctcccca gggaaactga actcagtttg catcagctgc tgcaacaccc ctctttgtaa 300 cgggccaagg cccaagaaaa ggggaagttc tgcctcggcc ctcaggccag ggctccgcac 360 caccatcctg ttcctcaaat tagccctctt ctcggcacac tgctgaagct gaaggagatg 420 ccaccccctc ctgcattgtt cttccagccc tcgcccccaa ccccccacct ccctgagtga 480 gtttcttctg ggtgtccttt tattctgggt agggagcggg agtccgtgtt ctcttttgtt 540 cctgtgcaaa taatgaaaga gctcggtaaa gcattctgaa taaattcagc ctgactgaat 600 tttcagtatg tacttgaagg aaggaggtgg agtgaaagtt cacccccatg tctgtgtaac 660 cggagtcaag gccaggctgg cagagtcagt ccttagaagt cactgaggtg ggcatctgcc 720 ttttgtaaag cctccagtgt ccattccatc cctgatgggg gcatagtttg agactgcaga 780 gtgagagtga cgttttctta gggctggagg gccagttccc actcaaggct ccctcgcttg 840 acattcaaac ttcatgctcc tgaaaaccat tctctgcagc agaattggct ggtttcgcgc 900 ctgagttggg ctctagtgac tcgagactca atgactggga cttagactgg ggctcggcct 960 cgctctgaaa agtgcttaag aaaatcttct cagttctcct tgcagaggac tggcgccggg 1020 acgcgaagag caacgggcgc tgcacaaagc gggcgctgtc ggtggtggag tgcgcatgta 1080 cgcgcaggcg cttctcgtgg ttggcgtgct gcagcgacag gcggcagcac agcaccttgc 1140 acgaacaccc gccgaaactg ctgcgaggac accgtgtaca ggagcgggtt gatgaccgag 1200 ctgaggtaga aaaacgtctc cgagaagggg aggaggatca tgtacgcccg gaagtaggac 1260 ctcgtccagt cgtgcttggg tttggccgca gccatgatcc tccgaatctg gttgggcatc 1320 cagcatacgg ccaatgtcac aacaatcagc cctgggcaga cacgagcagg agggagagac 1380 agagaaaaga aaaacacagc atgagaacac agtaaatgaa taaaaccata aaatatttag 1440 cccctctgtt ctgtgcttac tggccaggaa atggtaccaa tttttcagtg ttggacttga 1500 cagcttcttt tgccacaagc aagagagaat ttaacactgt ttcaaacccg ggggagttgg 1560 ctgtgttaaa gaaagaccat taaatgcttt agacagtgta aaaaaaaaaa aaaaaaaaa 1619 <210> SEQ ID NO 212 <211> LENGTH: 1010 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 212 ccgcagccgg gagcccgagc gcgggcgatg caggctccgc gagcggcacc tgcggctcct 60 ctaagctacg accgtcgtct ccgctggcag cagctgcggg ccccagcagc ctcggcagcc 120 acagccgctg cagcctgggg cagcctccgc tgctgtcgcc tcctctgatg cgcttgccct 180 ctccctggcc ccgggactcc gggagaatgt gggtcctagg catcgcggca actttttgcg 240 gattgttctt gcttccaagg ctttgcgctg caaatccagt gctaccagtg tgaagaattc 300 cagctgaaca acgactgctc ctcccccgag ttcattgtga attgcacggt gaacgttcaa 360 gacatgtgtc agaaagaagt gatggagcaa agtgccggga tcatgtaccg caagtcctgt 420 gcatcatcag cggcctgtct catcgcctct gccgggtacc agtccttctg ctccccaggg 480 aaactgaact cagtttgcat cagctgctgc aacacccctc tttgtaaccg ggccaaggcc 540 caagaaaagg ggaagttctg cctcggccct caggccaggg ctccgaacca ccatcctgtc 600 cctcaaatta agccctactt ctcggcacac tgctggaagc ttgaagggag aaggcaccca 660 ctcctgcata gtccatccag gcctcgcccc acacacccca ctccctgaga gagcacgccc 720 agggagacca aaaaccggga taggcaacgg acccccagac accacaaggg acccgaggac 780 aaagacgcag acaactcgcg aaagccaccc acgaatacaa cggcccgaac acagatataa 840 cgcacgagcc ccgaccgaca agagaagaag cagaagaaac acccacagac agaaacagac 900 accagcaaca agcgaaaaca gcaaaacgac actagcgaga caccacctgc acacaacacc 960 acagcccaac acagaggaca cgacaacaaa gagacagcac caacgacgaa 1010 <210> SEQ ID NO 213 <211> LENGTH: 480 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 213 gccaactccg gaggctctgg tgctcggccc gggagcgcga gcgggaggag cagagacccg 60 cagccgggag cccgagcgcg ggcgatgcag gctccgcgag cggcacctgc ggctcctcta 120 agctacgacc gtcgtctccg cggcagcagc gcgggcccca gcagcctcgg cagccacagc 180 cgctgcagcc ggggcagcct ccgctgctgt cgcctcctct gatgcgcttg ccctctcccg 240 gccccgggac tccgggagaa tgtgggtcct aggcatcgcg gcaacttttt gcggattgtt 300 cttgcttcca ggctttgcgc tgcaaatcca gtgctaccag tgtgaagaat tccagctgaa 360 caacgactgc tcctcccccg agttcattgt gaattgcacg gtgaacgttc aagacatgtg 420 tgagaaagaa gtgatggagc aaagtgccgg gatcatgtac cgcaagtcct gtgcatgatc 480 <210> SEQ ID NO 214 <211> LENGTH: 1897 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 214 gccaactccg gaggctctgg tgctcggccc gggagcgcga gcgggaggag cagagacccg 60 cagccgggag cccgagcgcg ggcgatgcag gctccgcgag cggcacctgc ggctcctcta 120 agctacgacc gtcgtctccg cggcagcagc gcgggcccca gcagcctcgg cagccacagc 180 cgctgcagcc ggggcagcct ccgctgctgt cgcctcctct gatgcgcttg ccctctcccg 240 gccccgggac tccgggagaa tgtgggtcct aggcatcgcg gcaacttttt gcggattgtt 300 cttgcttcca ggctttgcgc tgcaaatcca gtgctaccag tgtgaagaat tccagctgaa 360 caacgactgc tcctcccccg agttcattgt gaattgcacg gtgaacgttc aagacatgtg 420 tcagaaagaa gtgatggagc aaagtgccgg gatcatgtac cgcaagtcct gtgcatcatc 480 agcggcctgt ctcatcgcct ctgccgggta ccagtccttc tgctccccag ggaaactgaa 540 ctcagtttgc atcagctgct gcaacacccc tctttgtaac gggccaaggc ccaagaaaag 600 gggaagttct gcctcggccc tcaggccagg gctccgcacc accatcctgt tcctcaaatt 660 agccctcttc tcggcacact gctgaagctg aaggagatgc caccccctcc tgcattgttc 720 ttccagccct cgcccccaac cccccacctc cctgagtgag tttcttctgg gtgtcctttt 780 attctgggta gggagcggga gtccgtgttc tcttttgttc ctgtgcaaat aatgaaagag 840 ctcggtaaag cattctgaat aaattcagcy tgactgaatt ttcagtatgt acttgaagga 900 aggaggtgga gtgaaagttc acccccatgt ctgtgtaacc ggagtcaagg ccaggctggc 960 agagtcwgtc cttagaagtc actgaggtgg gcatctgcct tttgtaaagc ctccagtgtc 1020 cattccatcc ctgatggggg catagtttga gactgcagag tgagagtgac gttttcttag 1080 ggctggaggg ccagttccca ctcaaggctc cctcgcttga cattcaaact tcatgctcct 1140 gaaaaccatt ctctgcagca gaattggctg gtttcgcgcc tgagttgggc tctagtgact 1200 cgagactcaa tgactgggac ttagactggg gctcggcctc gctctgaaaa gtgcttaaga 1260 aaatcttctc agttctcctt gcagaggact ggcgccggga cgcgaagagc aacgggcgct 1320 gcacaaagcg ggcgctgtcg gtggtggagt gcgcatgtac gcgcaggcgc ttctcgtggt 1380 tggcgtgctg cagcgacagg cggcagcaca gcacctgcac gaacacccgc cgaaactgct 1440 gcgaggacac cgtgtacagg agcgggttga tgaccgagct gaggtagaaa aacgtctccg 1500 agaaggggag gaggatcatg tacgcccgga agtaggacct cgtccagtcg tgcttgggtt 1560 tggccgcagc catgatcctc cgaatctggt tgggcatcca gcatacggcc aatgtcacaa 1620 caatcagccc tgggcagaca cgagcaggag ggagagacag agaaaagaaa aacacagcat 1680 gagaacacag taaatgaata aaaccataaa atatttagcc cctctgttct gtgcttactg 1740 gccaggaaat ggtaccaatt tttcagtgtt ggacttgaca gcttcttttg ccacaagcaa 1800 gagagaattt aacactgttt caaacccggg ggagttggct gtgttaaaga aagaccatta 1860 aatgctttag acagtgtaaa aaaaaaaaaa aaaaaaa 1897 <210> SEQ ID NO 215 <211> LENGTH: 141 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 215 Met Trp Val Leu Gly Ile Ala Ala Thr Phe Cys Gly Leu Phe Leu Leu 1 5 10 15 Pro Gly Phe Ala Leu Gln Ile Gln Cys Tyr Gln Cys Glu Glu Phe Gln 20 25 30 Leu Asn Asn Asp Cys Ser Ser Pro Glu Phe Ile Val Asn Cys Thr Val 35 40 45 Asn Val Gln Asp Met Cys Gln Lys Glu Val Met Glu Gln Ser Ala Gly 50 55 60 Ile Met Tyr Arg Lys Ser Cys Ala Ser Ser Ala Ala Cys Leu Ile Ala 65 70 75 80 Ser Ala Gly Tyr Gln Ser Phe Cys Ser Pro Gly Lys Leu Asn Ser Val 85 90 95 Cys Ile Ser Cys Cys Asn Thr Pro Leu Cys Asn Gly Pro Arg Pro Lys 100 105 110 Lys Arg Gly Ser Ser Ala Ser Ala Leu Arg Pro Gly Leu Arg Thr Thr 115 120 125 Ile Leu Phe Leu Lys Leu Ala Leu Phe Ser Ala His Cys 130 135 140 <210> SEQ ID NO 216 <211> LENGTH: 443 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 185,208,304,339,348,386,421,428 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 216 cctttttttt tttttttctc agttattgac tggctgggtg tgacttagta cataagtact 60 caatattata aaaacctcaa ataattgact tgattttaca caacatcctt cccttttcta 120 caagttaatt tttttacaaa tcatttgggt tatctcctaa ataggttata ttttattgct 180 tctanaaaca atgtttcaaa atatatgngc attatcagta ataatttgta taaatatttc 240 ccacaacaat tttcataatt ttcaaagact aatttcttga ctgaagatat tttgctaggg 300 aagngaaact ttaaaatttt gagattttaa aaaaattgng tgaatggngg catgcaaagg 360 atttatatag tggctcccct aactgngtgc cgatcaggac acatattttt agacatctaa 420 ntctgganct taaatggagg gac 443 <210> SEQ ID NO 217 <211> LENGTH: 527 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 521,523 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 217 agacacaaca gtctgactat gagtgaggaa aatatctggg tcttttcgtc agtttggtgc 60 atttgctgct gctgttgcta ctgtttgcct caaacgctgt gtttaaacaa cgttaaactc 120 ttagcctaca aggtggctct tatgtacata gttgttaata catccaatta atgatgtctg 180 acatgctatt tttgtaggga gaaaatatgt gctaatgata ttttgagtta aaatatcttt 240 tggggaggat ttgctgaaaa gttgcacttt tgttacaatg cttatgcttg gtacaagctt 300 atgctgtctt aaattatttt aaaaaaataa atactgtctg tgagaaacca gctggtttag 360 aaaagtttag tatgtgacga taaactagaa attaccttta tattctagta ttttcagcac 420 tccataaatt ctattaccta aatattgcca cactattttg tgatttaaaa attcttacta 480 aggaataaaa actttaatat acaaaaaaaa aaaaaagggg ngnccgc 527 <210> SEQ ID NO 218 <211> LENGTH: 896 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 531,587,589,592,619,636,649,662,663,694, 723,729,735,737,741,752,783,816,817,819, 820,822,826,828,830,833,834,839,841,842, 869,892 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 218 gcagaacatt attttacaga cagcaaggat gcttctgagt gacacctagg aaattatttg 60 aagaaattct ttttatatct acacctgttg tgtaagaaac tttaaaacat tggttatttt 120 ctcacctttt tttctaattc actttgattg ctaggggtca tgtatgcttc gaagttacag 180 gactaaaaga gcaaactgac cggcctaaaa ctaaaatgac atttattccc tagctacaaa 240 catcagcgtt attatgttaa ttataccttg ccctctatca ttataaatgg ttgccatggt 300 gtttctaaaa ataagtgttt taccattaat gtgtagaggg caaacaaagc ataaagtact 360 aagggatcat gcttatccta gggtctcaca gaagagagga catatttaat taatcttgtg 420 aattacagaa caggttgtgg tccagacacc aagaatcata ggggtttttt tttaaaaaac 480 ctaatagaag tagggggacc tctctctttg gctaagagtc taaaggaagg naggcatctg 540 tttaattagt tggttcaccc tggctttacc tctggttaat gctttgngnt antaggaagg 600 aaaaatcctt tatcttttnt tccaagccct ccctgnctga cttacccana ctgggattac 660 cnngaaaccc cagggggatt tatgggggga gaanggattt tttcaccctt taaacctctt 720 aanccccang gggananaaa ncctcttggg anagcctatg gccctatttt ttaatatcca 780 ggnccccttg gaaaactttt ttttttttaa aagccnntnn antttnantn aannaaaana 840 nncaaccttt tggccccaaa aaaaaaggnc cccccctaag gcccccaccc tntttt 896 <210> SEQ ID NO 219 <211> LENGTH: 770 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 525,527,574,619,628,730,752 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 219 aaagaaggtt cacttccatt acagtatgag tggcaaaaat tgtctgactc acagaaaatg 60 cccacttcat ggttagcaga aatgacttca tctgttatat ctgtaaaaaa tgcctcttct 120 gagtactctg ggacatacag ctgtacagtc agaaacagag tgggctctga tcagtgcctg 180 ttgcgtctaa acgttgtccc tccttcaaat aaagctggac taattgcagg agccattata 240 ggaactttgc ttgctctagc gctcattggt cttatcatct tttgctgtcg taaaaagcgc 300 agagaagaaa aatatgaaaa ggaagttcat cacgatatca gggaagatgt gccacctcca 360 aagagccgta cgtccactgc cagaagctac atcggcagta atcattcatc cctggggtcc 420 atgtctcctt ccaacatgga aggatattcc aagactcagt ataaccaagt accaagtgaa 480 gactttgaac gcactcctca gagtccgact ctcccacctg ctaangnagc tgcccctaat 540 ctaagtcgaa tgggtgcgat tcctgtgatg attncagcac agagcaagga tgggtctata 600 gtatagagcc tccatatgnc tcatctgngc tctccggggt cctttccttt ttttgatata 660 tgaaaaccta ttctgggcta aattgggtac tagcctcaaa tcatcaaaaa ataagttaat 720 caggaactgn accgaaaata ttttttaaaa anttttgttt gggtatattc 770 <210> SEQ ID NO 220 <211> LENGTH: 892 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 2,3,208,321,337,542,551,560,590,606, 613,614,620,639,640,645,646,652,659,661, 663,666,676,679,707,708,709,717,718,719, 726,728,730,732,738,742,751,764,773,777, 782,792,821,825,827,828,831,832,833,870, 880 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 220 tnnacactca ccgccctcgc cgccgcgcca tggacgcccc caggcaggtg gtcaactttg 60 ggcctggtcc cgccaagctg ccgcactcag tgttgttaga gatacaaaag gaattattag 120 actacaaagg agttggcatt agtgttcttg aaatgagtca caggtcatca gattttgcca 180 agattattaa caatacagag aatcttgngc gggaattgct agctgttcca gacaactata 240 aggtgatttt tctgcaagga ggtgggtgcg gccagttcag tgctgtcccc ttaaacctca 300 ttggcttgaa agcaggaagg ngtgcggact atgtggngac aggagcttgg tcagctaagg 360 ccgcagaaga agccaagaag tttgggacta taaatatcgt tcaccctaaa cttgggagtt 420 atacaaaaat tccagatcca agcacctgga acctcaccca gatgcctcct acgtgtatta 480 ttgcgcaaat gagacggtgc atggtggtgg agtttgactt tatacccgat gtccagggag 540 cnagtactgg ntttgtgacn tgtcctcaaa ctttcctgtc caagccaggn gggatgtttt 600 cccaantttg ggnnggtgan ttttttgctg gggggcccnn aaaannaaat gnttggggnt 660 ncntgncttt gggggnccna ccccgggggg gcggaaattg gttcccnnnc gggaatnnna 720 accccntngn cngggggngg gntttttggc nccccttccc cggnaaaagg cgnggcnccc 780 cnttcggggg gncccttggg ggaaaataaa ccaaaggggt nggcncnngg nnntttgggg 840 gaaacacacc gagcgcttcc ctttttgttn acccaacaan gggccctttc ca 892 <210> SEQ ID NO 221 <211> LENGTH: 629 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 408,502,507,540,542,545,550,562,572,576, 623,628 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 221 cctttttttt tttttttggt acaaattatg taaaacattt gtgctaagaa cttttctccc 60 tccccaaacc aaaaagaaaa taaaaaataa aaaaattaaa aaaattaaaa attgagtatt 120 ctaactacag ctcaacaatt gaatcaaatg tcactgtttt gtaaatactt tatccataac 180 gaaagatata aacatgcaaa aaacctgaat ccatagtcca aataatacat acacatgttc 240 tgaagtttct gcacttctcc atagactatg ccaataaaac attatgtaca catactattt 300 ttacagtgaa gtggaaaaat acagaaataa aaaagtgtac atggattaag accaaaatgt 360 gtctaacatt ctagtttatg aaaaaattca attttgctac aaattggnga tatgaaaact 420 ccctttattt gcaaccagct gagtaagttt taagatttta gtgaaaaaaa aaaaaaacaa 480 actaaagtct aaaactagaa gnaatgngca ttttccaatc tcatgggctc atcccccaan 540 anaanaaaan cgctccatga gnttttttgg tnggtnaatt ttggatttta aaaaaagcaa 600 atgcaatgta acaaaagcgg ggntgaanc 629 <210> SEQ ID NO 222 <211> LENGTH: 763 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 626,628,634,661,748,751 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 222 ggaagtgctg aatggtgttg gcaggggtat taaacgtgca tttttactca actacctcag 60 gtattcagta atacaatgaa aagcaaaatt gttccttttt tttgaaaatt ttatatactt 120 tataatgata gaagtccaac cgttttttaa aaaataaatt taaaatttaa cagcaatcag 180 ctaacaggca aattaagatt tttacttctg gctggtgaca gtaaagctgg aaaattaatt 240 tcagggtttt ttgaggcttt tgacacagtt attagttaaa tcaaatgttc aaaaatacgg 300 agcagtgcct agtatctgga gagcagcact accatttatt ctttcattta tagttgggaa 360 agtttttgac ggtactaaca aagtggtcgc aggagatttt ggaacggctg gtttaaatgg 420 cttcaggaga cttcagtttt ttgtttagct acatgattga atgcataata aatgctttgt 480 gcttctgact atcaatacct aaagaaagtg catcagtgaa gagatgcaag actttcaact 540 gactggcaaa aagcaagctt tagcttgtct tataggatgc ttagtttgcc actacacttc 600 agaccaatgg gacagtcata gatggngnga cagngttaaa cgcaacaaaa ggctacattt 660 ncatggggcc agcactggca tgagcctccc taagcttttt tgaagaattt taagccctgg 720 taaattaaaa aaaaaaaaaa aaaagggngg nccccctcca aat 763 <210> SEQ ID NO 223 <211> LENGTH: 885 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 21,571,599,653,714,717,746,755,756,761, 762,781,782,790,814,849,884 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 223 tggagccgct gtggttgctg nccgcggagt ggaagcgcgt gcttttgttt gtgtccctgg 60 ccatggcgct gcagctctcc cgggagcagg gaatcaccct gcgcgggagc gccgaaatcg 120 tggccgagtt cttctcattc ggcatcaaca gcattttata tcagcgtggc atatatccat 180 ctgaaacctt tactcgagtg cagaaatacg gactcacctt gcttgtaact actgatcttg 240 agctcataaa atacctaaat aatgtggtgg aacaactgaa agattggtta tacaagtgtt 300 cagttcagaa actggttgta gttatctcaa atattgaaag tggtgaggtc ctggaaagat 360 ggcagtttga tattgagtgt gacaagactg caaaagatga cagtgcaccc agagaaaagt 420 ctcagaaagc tatccaggat gaaatccgtt cagtgatcag acagatcaca gctacggtga 480 catttctgcc actgttggaa gtttcttgtc atttgatctg ctgatttata cagacaaaga 540 tttggttgta cctgaaaaat gggaagagtc nggaccacag tttattaccc aattctgang 600 aagtcccgcc ttcgttcatt tactactaca atccacaaag taaatagcat ggngggctac 660 aaaaaattcc tgtcaatgac tgaggatgac atgaaggaaa aaaatggaaa ttgnaanttt 720 tgaaaagggg gtttcctgaa aacagncatc tatanntgga nnttggttta tttcattggg 780 nnaatttttn cctggggggg aaaaacccca aaanggatac ctttactgga accggggggg 840 gaaattggnc ctttttattt tttttttggg cccccaattt tggnc 885 <210> SEQ ID NO 224 <211> LENGTH: 541 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 300,311,350,422,490,508,526 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 224 cctttttttt tttttttaaa acaaacttaa ctttatttcc tcactttcac ttaaaacttg 60 attttataaa acacatgaaa aaacattttt aagagttctg tatcacagaa cattaaacag 120 tacaaatatc cattgcttca taggttcaag ttacataaat taaagtcaaa taattggaaa 180 ctgattcaat agggaaaact atacatgaaa tgaaggtcaa aaggagctat acagcaatat 240 ttcattggtt atagattatg agttactttc aggaccttaa caaagattct gaatatttan 300 acttcctttg ntggatttta tacttaaata tctccctacc tatactgagn caaactactt 360 gaccaaaaca tctgatttag gaaagcatct agctttatag cacaagtttt tccatctaca 420 gntactatct tcaaaggaat atacatcaca atgttgacaa aaaaacctcc tggttccttt 480 tgaacaatgn gcaataaatt catgatgnta accccatggg gaaggncaaa aaggggaccc 540 a 541 <210> SEQ ID NO 225 <211> LENGTH: 543 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 23,226,295,316,327,345,428,445,476,479, 521,522 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 225 cctttttttt tttttttgta agnttaaatt tattttttaa aaatgcttgt cttcctcact 60 agacaatcaa ctctatgagg gcagagacta tgtcaccact gtcccaccag cccctggcac 120 acagtaggta ctcaataaat atatgttgga aggatggatg gaggtaatgg atggaaagat 180 ggatggaagg atgaatggag ggatggatgt gacccagctg aagtgngagt aggaacattc 240 tcttattatg ggtggaggaa agagagagga gattgagaaa ataagataaa atacnttgat 300 gagcatcatt tttggngttc gaaaagnagg attgaattag gactnataaa tctagagaat 360 tttacctctt tcaatgccca agccacactt ttctatcact ttgaaaccga aaaagaaata 420 ctttcccnac atttgctttg ctggnaggaa atgctttaat aaaaatgcaa tctctnagnt 480 gccatggcat cattaaaaga aaggatgtca tgcccaggcc nnaacttgaa ggggggaggc 540 ccc 543 <210> SEQ ID NO 226 <211> LENGTH: 703 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 530,535,560,567,584,600,664,671 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 226 tgttaatgca attatagaaa tacatcggag acacaacatg atgtggccat tacaggtttc 60 ataaaattac actgacttgg ctgttacttg atcttaggaa acagcacagt ttaagatatt 120 gtgaattctg acttatactt tattaaatgc tataaatcta aatagatcct gttggatgtg 180 atgggtctag tccagtttat ttaagttcat gtttcactgt ttgcactttg cattgaacaa 240 tgggtttatt cgctgatgta aacggttcga gtgaagaatt aatgcagtaa gtatgacaac 300 acatacacac ttgcctctcc ccatctccag aagaggggag cagagtccga gcttatctaa 360 atatgaatgt ggccacaaag ctgtggaagg tgacaaagct taaacacctt tgccctggct 420 ctgcattgtc acctagagag caagaggtct atagaaacat catgtcacat gaaacgattc 480 tctgcttttt ggtctgaact tgaaggccct aaactgcaaa atctaagagn tgggngggta 540 ttaaaatgct tttaaaaagn taactgnggc accaattcta atgnaatccc acttgggacn 600 gggttttttt ggtttggttt ggttttgggg gggggggggg gggggccctg ggaaaagggg 660 aacnaacatg nttttgaaat acatattggg aaaaaaaatg ggg 703 <210> SEQ ID NO 227 <211> LENGTH: 501 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1,5,154,239,281,292,336,421,459,470 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 227 ngtgnccctg gccatggcgc tgcagctctc ccgggagcag ggaatcaccc tgcgcgggag 60 cgccgaaatc gtggccgagt tcttctcatt cggcatcaac agcattttat atcagcgtgg 120 catatatcca tctgaaacct ttactcgagt gcanaaatac ggactcacct tgcttgtaac 180 tactgatctt gagctcataa aatacctaaa taatgtggtg gaacaactga aagattggnt 240 atacaagtgt tcagttcaga aactggttgt agttatctca natattgaaa gnggtgaggt 300 cctggaaaga tggcagtttg atattgagtg tgacangact gcaaaagatg acagtgcacc 360 cagagaaaag tctcagaaag ctatccagga tgaaatccgt tcagtgatca gacagatcac 420 ngctacgggg acatttctgc cctgttggaa ggttcttgnt catttgatcn gctgatttat 480 acagacaaaa gatttggttt g 501 <210> SEQ ID NO 228 <211> LENGTH: 539 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 3,13,101,405,440,456,465,513,526 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 228 ggnttatact gcnaaagtta tgcattacac catattcagt tggtaacata aaccgagata 60 taagaattta tatattggct tctggttatt ttcttagcac nggagtgcct tttccaacca 120 ttgagtgcat gatcagatta cacaaataca agcacatatc atgtgttctc ccatgagaca 180 ttattcactt aggattgtct acaataaaaa aagttaaagt acaagcaata ataaattcat 240 aagaattttt tgaatttaaa ataaatgcat gtgtctttga gaacatttct tttgaaattc 300 atatttttaa aaataacaag tttcttaaat cagtctttta gtcgtgtttt catatggtat 360 ttatcagtag gtggaaacac ttcacatcat ttaaccccaa aaggnataat aattaaactg 420 caattaaagg gaggaacagn tgaatcatta caacantaat acggngtaca aatcagagtt 480 ggccacacaa tacacatgtg taatactgga aanaaataca atatcngaat cctggatgg 539 <210> SEQ ID NO 229 <211> LENGTH: 790 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 576,622,678,706,738,755,766 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 229 cagagagcat gatcagtgct gatactgaca agtacttttt taccttaaaa tcaacttcta 60 tggaactaca agatcaatct agctcccgag tgacattttc cattgtctgt aataatgccc 120 tcggatgagt tgtgtctaaa attaagttca tctttattta tatgcgaact taactgccat 180 agtccctaat gtattgcgtt tgtaacctga tcgtattatg tttacagctg aaagatttca 240 tctagacatg tctttcgtcc ttattattca aagtgtaatt gaaagagata tttagtatta 300 agacatgttc cccaattgag aattttccag aatattctac ttaagaagaa gaagagcaat 360 taactgcctt tagtgtaagg gcgagagtgc atagaaatat gcaatgtaaa atgtttgcat 420 gaattatttc acatcatgta agctttccca tattcataag atgaacacta tagaagtctc 480 atttctctgt gatcttctgc cattaggaaa gtaaggagat tggtatctat atctagtctc 540 ctttccatat tgaactgcat ggctctaatc ctcagnggat ttttatccct tctccggtta 600 tttaaaattt gccctattta anctggaagc ctggataaac tgctgagccc cgaatattcc 660 tggggattgg gagtttantt gctgggagaa ccacttggtt gaagancacc atttttttcc 720 cttttttttc tttttccnga attttttccc tcaanccatt ggtttnctct taaatggaaa 780 aacccccccg 790 <210> SEQ ID NO 230 <211> LENGTH: 744 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 603,618,636,723,724 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 230 aaattttatg ggtgggtgcc aaatactgct gtgaatctat ttgtatagta tccatgaatg 60 aatttatgga aatagatatt tgtgcagctc aatttatgca gagattaaat gacatcataa 120 tactggatga aaacttgcat agaattctga ttaaatagtg ggtctgtttc acatgtgcag 180 tttgaagtat ttaaataacc actcctttca cagtttattt tcttctcaag cgttttcaag 240 atctagcatg tggattttaa aagatttgcc ctcattaaca agaataacat ttaaaggaga 300 ttgtttcaaa atatttttgc aaattgagat aaggacagaa agattgagaa acattgtata 360 ttttgcaaaa acaagatgtt tgtagctgtt tcagagagag tacggtatat ttatggtaat 420 tttatccact agcaaatctt gatttagttt gatagtgtgt ggaattttat tttgaaggat 480 aagaccatgg gaaaattgtg gtaaagactg tttgaccctt catgaaataa ttctgaagtt 540 gccatcagtt ttactaatct tctgtgaaag catagatatg cgcatggtca cttttattgg 600 ggncttataa ttaaatgnaa aattgaaatt catttntgtt caaaggggat atcttccaat 660 agccttttta gtagtattca aatatcagtc tatggataat gattttattt ctttcttagg 720 agnntcaatg tggactaatt cagt 744 <210> SEQ ID NO 231 <211> LENGTH: 797 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 429,446,495,523,537,626,628,642,664,707, 711,713,727,733,786,793 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 231 gtgccgcctc caaagagccg tacgtccgct gccagaagct gcataggcag taatcattca 60 tccctggaat ccatgtctcc ttccaacatg gagggatatt ccaagactca gtataaacaa 120 gtaccgagtg aagactttga acgcactcct cagagtccaa ctctcccacc tgctaaggta 180 gctgccccta atctaggtcg aatgggcgtg attcctgtga tgattcccgc acagagcaag 240 gatgggtcta tagtatagag cctccatacg tctcatctgt gctttccgtg ttcctttcct 300 tttttgatat atgaaaacct attctggtct aaattttgtt actagcctca aaatgtatcc 360 aaaaataagt taatcaggag ctgtaaggaa tatatttttt aaaatttttc tttggttata 420 tcgaaatang ttacaggcat taaagntagt aaagacaagt ttaccatctg aaaaagctgg 480 atttctttaa gaggntgatt ataaagggtt ctaaatttat cantacctaa gtaagangta 540 gcacttttga atatgaaatc ataagtgaag acattggtga acttacttgc atacccaagt 600 tgatactttg agtaaccatc tgaaangngg gacttggata anttttacca ttatttttaa 660 gganggggat cttaattatt tatgggcccc cagtctcccc cccaaantaa ntnccgaaaa 720 cattccnttg acnaaaatta ccccctgggg gggggttgga cctttggttt tcccaggttt 780 cttggnaaaa ctntggg 797 <210> SEQ ID NO 232 <211> LENGTH: 635 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 501,531,556,623,633 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 232 tattattagg atggtaagag tattataagg attggtacaa ggcatgatga gtccttttgc 60 ttttaggctt ttgacttctg gttttagact ttctttagct tctgttgtta gacaacattg 120 tgcaagcttg gtttttataa gtttgcatgg attaaactga acttaatgaa attgtccctc 180 cccccaaatt ctcagcacaa tttttaggcc cacaaggagt caagcacctc aaggagatct 240 tcagtttgaa cttggtgtag acacagggat actgatgaat caatattcaa attagctgtt 300 acctacttaa gaaagagagg agaccttggg gatttcgagg aagggttcat aagggagatt 360 ttagctgaga aataccattt gcacagtcaa tcacttctga ccaagttatc agaaaaagga 420 gaaaagaatg tctccccact aaatgttcta gggtggtgag aaatctaggg tgggtatcta 480 aatcacaata tttggatatt ncaatatcta aatattggtg gaaatactct nctgaagtgt 540 cattgactct aaaaanacac ttgtgatcat ggcaggggtt aaggtcattt ttattcctat 600 aatccttata ttaacaattc ctntgattaa ganaa 635 <210> SEQ ID NO 233 <211> LENGTH: 663 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 429,432,437,475,485,491,493,535,550,555, 571,612,640,653 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 233 cctctgtata gaaatctaaa agaattttac cattcagtta attcaatgtg aacactggca 60 cactgctctt aagaaactat gaagatctga gatttttttg tgtatgtttt tgactctttt 120 gagtggtaat catatgtgtc tttatagatg tacatacctc cttgcacaaa tggaggggaa 180 ttcattttca tcactgggag tgtccttagt gtatgaaaac catgctggta tatggcttca 240 agttgtaaaa atgaaagtga ctttaaaaga aaatagggga tggtccagga tctccactga 300 taagactgtt tttaagtaac ttaaggacct ttgggtctac aagtatatgt gaaaaaaatg 360 agacttactg ggtgaggaaa tccattgttt aaagatggtc cgtgtgtgtg tgtgtgtgtg 420 tgtgtgtgnt gngttgngtt ttgtttttta agggagggaa tttattattt accgntgctt 480 gaaantactg ngnaaatata tgtctgataa tgatttgctc tttgacaact aaaantagga 540 ctgtataagn cctanatgcc tcctgggggg ntgatcttac aagatattgg tgatacccct 600 ttaaaaattg gncccccggc atttttcccc tttgcttctn caaattaaaa ggnctttttc 660 cca 663 <210> SEQ ID NO 234 <211> LENGTH: 873 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 20,29,58,603,630,652,678,711,715,745, 752,756,766,774,789,820,823,840,873 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 234 acttggggat tctcatgttn atggatacng tttggcaatc actacattga atgtagtntt 60 ttaaaaaaat taacttatgc tattagttga cccatcattg ctaattttgg cccacacagt 120 gtttgcatta caaaaacctg ttctttactt cctagtcttg tttcagtctt aatatcagaa 180 gttcttgagt tcaaaataag cacaacatgt catccaggga tggctagctt gtttgggatt 240 catctaaact gctggcaata tctagacaaa aacattccac agtccagcta atatggttgt 300 cacaactctt gaaaagggcc caacatctgg atggcaagtg aaaatgtgat cagggtttaa 360 gaactaccca ctaataaata aacatggagc tatttccatg tcttgggtgt tgtgtttcta 420 agaagagaca gcctttccat cagaaaattt ctgggaggga agaaaaagaa cagttttgat 480 gaattcgctt tgcaaatcat catccaatgt tctttgtaac cagaaaggtt ttcttctgct 540 ttcttgcagc tggtatactt tctgctgagt gccctggggc ctgacggtct gtgtgctggc 600 cgnggccttt gcccgcccac cactattcgn cagctcacac cagtttacct gngagacccc 660 ctccgacttt tggccagngc aaactggccc cttccttcgg gagccggctc nagcnaggac 720 ccttttggtt ttacccgggg atggngaccg gnctgnaccc agccgnccac tggncccttt 780 tcaaacctng ttcctttccc tcatccccag aaggaatttn ttnaaatttt gggccttggn 840 ggcccttggg ggggcctttg ggttgggccc ctn 873 <210> SEQ ID NO 235 <211> LENGTH: 51 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 26,48 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 235 tttttttttt ttttttttta attttngttt tttttttttt tttttttngg g 51 <210> SEQ ID NO 236 <211> LENGTH: 765 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 540,555,590,593,670,685,708,711,714,733, 760 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 236 ggagacctaa tgtttcatat gcagcgacaa agaaaacttc ctgaagaaca tgccagattt 60 tactctgcag aaatcagtct agcattaaat tatcttcatg agcgagggat aatttataga 120 gatttgaaac tggacaatgt attactggac tctgaaggcc acattaaact cactgactac 180 ggcatgtgta aggaaggatt acggccagga gatacaacca gcactttctg tggtactcct 240 aattacattg ctcctgaaat tttaagagga gaagattatg gtttcagtgt tgactggtgg 300 gctcttggag tgctcatgtt tgagatgatg gcaggaaggt ctccatttga tattgttggg 360 agctccgata accctgacca gaacacagag gattatctct tccaagttat tttggaaaaa 420 caaattcgca taccacgttc tctgtctgta aaagctgcaa gtgttctgaa gagttttctt 480 aataaggacc ctaaggaacg attgggttgt catcctcaaa caggatttgc tgatattcan 540 ggaccccgtc tttcnaaatg ttgattggga tatgatggac aaaaacaggn ggnaccttcc 600 tttaaccaaa tatttctggg gaatttgggt ttggacacct ttgattctca atttactaat 660 ggaacctggn ccagctcact cccanaatga cgaatgacct ttggggangg naanaattgg 720 gatcaagtct ggnaattttg gaaagggttt ttggaggtan tattc 765 <210> SEQ ID NO 237 <211> LENGTH: 739 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 460,478,485,509,527,529,554,573,575,578, 603,607,609,616,621,643,651,674,675,689, 696,729 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 237 ctctactgga agtttgaccc tgtgaaggtg aaggctctgg aaggcttccc ccgtctcgtg 60 ggtcctgact tctttggctg tgccgagcct gccaacactt tcctctgacc atggcttgga 120 tgccctcagg ggtgctgacc cctgccaggc cacgaatatc aggctagaga cccatggcca 180 tctttgtggc tgtgggcacc aggcatggga ctgagcccat gtctcctcag ggggatgggg 240 tggggtacaa ccaccatgac aactgccggg agggccacgc aggtcgtggt cacctgccag 300 cgactgtctc agactgggca gggaggcttt ggcatgactt aagaggaagg gcagtcttgg 360 gcccgctatg caggtcctgg caaacctggc tgcctgtctc catccctgtc cctcagggta 420 gcaccatggc aggactgggg gaactggagt gccttgctgn atccctgttg ggagggtnct 480 ttcangggct ggcactgaaa caaaggggnt gggggcccat gggcttnanc ctgggtgaac 540 aactgggctt gtanggcaag ggcactttct gangncangg cttgggaagg ggcctgcatc 600 tgnctgncnt tttggntgac naatcctggg aaatctggtt ttnccaaaat nccaggccaa 660 aaaagtttac cagnncaaaa tggggggang ggggantttt ttttatggca aggaaaaaac 720 ccccagggnc ccttgggaa 739 <210> SEQ ID NO 238 <211> LENGTH: 818 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 311,378,441,442,494,505,520,525,540,545, 551,570,600,602,616,619,639,641,650,656, 671,684,686,697,701,724,726,732,738,749, 759,762,792,797 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 238 cctggtgatc gcttcagtag agatgtctgg tgatatggtg aactgatcag gccctgacat 60 ggatgttccc ctagaggata tcacttctgt cctggagacc tcagtggtag caccactggg 120 cacttcagaa aggacagtgc ttccctctgt ggctgagctg gtcccttcag agccgctgga 180 ctccctcaat ccaggggtca gggaggaagc tagctctgtc tgaatcctcc tagtctcaag 240 gaaggcagga gttgatgtga gaacacttgt atcccccatg gtggaggtgg tacacattgg 300 agatgagtca nctaggacag aggactgtga tttatatcca gagctggtgg ttgccacatt 360 ggtccctcct gtgtttgngg aaggatgcac ggcttctgta tgtgcagtgt ctttgtaagt 420 ggtaagtctc tcatgggagg nngggctcaa acttgaagat gaactggttc caggttcttg 480 tgcttgtacc caanatatct gtggntgtcc ccggccagan ggganaaagt gaagtcacan 540 ggaangggaa naggggggga tatgtgctan gaatgtggtg gaaaacaagg atgaagtgan 600 gncccggcag gtaaanacna gcgggggaag gaatggaang ncttggtttn ttttcncaaa 660 agggaagggc ntaggccaat gacncnccct cccgganctt ntgcccattg ggaagggggc 720 attntnttgg gngggggnaa aatccctgna attaactana anaaaggggg tttccccccc 780 aaaaaggggg gnggttnctt ggggttcaaa ataaaggg 818 <210> SEQ ID NO 239 <211> LENGTH: 829 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 207,379,714,717,736,762,770 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 239 ctggtcttgg actcctgacc tcaagtgatc cacccccctc agcctcccaa agtgctagga 60 ttacaggcat gagtcactgc gtcaggccaa aattctgtat tttcaattag agtcaaagcc 120 caaggatgtc tctaccatct tgtagccctt gccaatagcc tactcttgtc ttccagggtt 180 cctccaaatc tctctccaaa tatttgntat ctactcattc aatacccttc ttcaaccatc 240 ctcttgcttt ggaattgaca tgaaccaact aggcccgcct tattggtagg aattcatttg 300 ccctgcctgc cagcccccat agagacagaa ccattgccta gtgaaagaag attttaatga 360 cgtgatgaaa atattttana aagcaccttg aagattagta tttttatgta acttctgttg 420 gagagatgtc ttcaggagac tgaagtagaa gagcgactgt caaaatggaa agtcccagag 480 acatccaatt tatgtaaatc aacatcacct gaattcagaa tctcatccag atttcaacaa 540 agacttctga atgccaacca aagaagagga ctgaatttac agactctcac tctaacaata 600 tatgctggtc aatttgaaaa acagaataaa attattttgg caagaaactg gatttttaat 660 ggacatatat tggtttaaaa tggtaccaac tttttatttt taccccattt tggnggnaaa 720 aaacccgggg aataanggga aaagcaaaag ggaaaatata tncaaatatn gggaaggttt 780 ttacctttaa ttttggttca ttaaacctaa cccagaaggc caaacaatt 829 <210> SEQ ID NO 240 <211> LENGTH: 177 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 240 cctttttttt tttttttaca tacaaaatgt tttaattgag aaaaaaattc aaaacagtca 60 cacatatcca ttatcatcat ggttctctga aatattttct tatacaaatg aaatatttaa 120 aatggaaaaa ttacattttt caaatctaat taactaatta tttttgtcct ggtcgac 177 <210> SEQ ID NO 241 <211> LENGTH: 591 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 96,152,212,246,280,403,436,491,494,501, 519,568,579 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 241 cctttttttt ttttttcatt aaataatcca tcatcacatt agtacaatac aattttatat 60 tttttaaata tactatatat gttaaggata aggggngaag ttttcttcct ttgtaatacc 120 tgttcaagag tttaatggat taggagatta gngttaacct tgaggataaa agtacaaatt 180 tgtctcatta ggacacttct accaagcatt tnttaaggct atagtttaac atttggtttc 240 aaaaanaaaa aaaaaggttt catttaaaaa ataatttagn gaattacatt ctttcataac 300 ttccacccta attagttaca aagataagtc taaagattct tagttttggg tactaattta 360 catttatatt taaagattaa ttttacttgg atcttaaaac aanaatttta tgttggaaaa 420 aagagaacta aatacntttg tataaaggct gtaaatgtcc catggcaaat gctctgtctc 480 aatattttct nccncaatta naaacagggc tctgcaaana gagacttggg ttgttcaggt 540 tcacctttcc cgaggaattg ggggctgnca tctgaaganc atagagaaac a 591 <210> SEQ ID NO 242 <211> LENGTH: 924 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 102,104,591,592,595,596,640,641,650,683, 706,708,720,734,735,757,759,779,791,804, 806,825,837,905,912 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 242 aacctttcag gaaaatccaa ggaaatacag aagcaaggca gcaccatagt cttcccagcc 60 aaggtggaag tgcctctggt tcctccagca attcccactg gngntatcat aactcaacag 120 tctgttgcaa tcagttgtag aaaggcacag agtgacagct ggaatgcaaa gaaatgtgca 180 caacccagag ctctgtcagc cttgccaaaa ctcaagtgcc cccatgggag ggtcttgcaa 240 catatgttct gttgagcaaa gaggttgcaa accaagcggt tattgcaata aacaccactt 300 gtgacaaaca aagtttgtaa gtttaaattt attttttaaa aatgcttgtc ttcctcacta 360 gacaatcaac tctatgaggg cagagactat gtcaccactg tcccaccagc ccctggcaca 420 cagtaggtac tcaataaata tatgttggga aggatggatg gaggtaatgg atggaaagat 480 ggatggaagg atgaatggag ggaatggatg tgacccagct gaagtgtgag taggaacatt 540 ctcttattat gggtggagga aagagagagg agattgagaa aaataagata nnatnncatt 600 ggatgaagcc atcatttttt ggggggttcc gaaaaaagtn ngggatttgn aaatttaagg 660 gaacttaaat aaaaatcctt aanaaaaaaa atttttttaa cccctncntt tttccaaaan 720 gggcccccca aaanncccca acccaacttt ttttttncnt tatttccacc ttttttggna 780 aaaaaccccc naaaaaaaaa aggntnaaaa attacccctt ttttnccccc aaacccnttt 840 ttggcctttt tgccttgggg aaagggaaaa aaggcttttt aaataaaaaa aatggccaat 900 tcttnttaaa anttggccaa tggg 924 <210> SEQ ID NO 243 <211> LENGTH: 278 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 211,276,277 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 243 cctttttttt tttttttaag atttaactct gaatacaaat gtattttttt cttcttctct 60 ccctacatat attctaaacc ttctaaagtt tttttatttt tttaaggatc actttatcat 120 aaaataaaat atccttttca tataataaat tacctaataa aaagtctttt tttttcatat 180 tagcccaggt tctttgctac atttatatgg naataaacgc ctttattaaa atagaatatt 240 aaattataaa gaactgcttt tttttttttt ttttgnna 278 <210> SEQ ID NO 244 <211> LENGTH: 3072 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 244 gcgcagacgc cccagccccc caccgccccc aaaggggcga gcgacgccaa gctctgcgct 60 ctctacaaag aggccgagct gcgcctgaag ggcagcagca acaccacgga gtgtgttccc 120 gtgcccacct ccgagcacgt ggccgagatc gtgggcaggc aaggctgcaa gattaaggcc 180 ttgagggcca agaccaacac ctacatcaag acaccggtga ggggcgagga accagtgttc 240 atggtgacag ggcgacggga ggacgtggcc acagcccggc gggaaatcat ctcagcagcg 300 gagcacttct ccatgatccg tgcctcccgc aacaagtcag gcgccgcctt tggtgtggct 360 cctgctctgc ccggccaggt gaccatccgt gtgcgggtgc cctaccgcgt ggtggggctg 420 gtggtgggcc ccaaaggggc aaccatcaag cgcatccagc agcaaaccaa cacatacatt 480 atcacaccaa gccgtgaccg cgaccccgtg ttcgagatca cgggtgcccc aggcaacgtg 540 gagcgtgcgc gcgaggagat cgagacgcac atcgcggtgc gcactggcaa gatcctcgag 600 tacaacaatg aaaacgactt cctggcgggg agccccgacg cagcaatcga tagccgctac 660 tccgacgcct ggcgggtgca ccagcccggc tgcaagcccc tctccacctt ccggcagaac 720 agcctgggct gcatcggcga gtgcggagtg gactctggct ttgaggcccc acgcctgggt 780 gagcagggcg gggactttgg ctacggcggg tacctctttc cgggctatgg cgtgggcaag 840 caggatgtgt actacggcgt ggccgagact agccccccgc tgtgggcggg ccaggagaac 900 gccacgccca cctccgtgct cttctcctct gcctcctcct cctcctcctc ttccgccaag 960 gcccgcgctg ggcccccggg cgcacaccgc tcccctgcca cttccgcggg acccgagctg 1020 gccggactcc cgaggcgccc cccgggagag ccgctccagg gcttctctaa acttggtggg 1080 ggcggcctgc ggagccccgg cggcgggcgg gattgcatgg tctgctttga gagcgaagtg 1140 actgccgccc ttgtgccctg cggacacaac ctgttctgca tggagtgtgc agtacgcatc 1200 tgcgagagga cggacccaga gtgtcccgtc tgccacatca cagccacgca agccatccga 1260 atattctcct aagccccgtg ccccatgcct ccggggccca ctccactggg cccaccctgg 1320 acctgttttc cactaaagcc ttttggaaag cggtgatttg aggggcaagg tgcttagaga 1380 tactcgctcg ctggggaagg ggggagggag gcagtggtgg ctggagggtg cgccactttc 1440 agagcctctg gtcaccctgt cctggaaaga ttgggagggg gccagactga aaattttact 1500 agagttacaa ctctgatacc tcaacacacc cttaaatctg gaagcagcta agagaaactt 1560 ttgttttgcc agaggtggcc actaaggcat tctgacgccc tctgcccacc tcccccgctg 1620 tgtgtcactc caccccttct tccgaggagg gggtgggtaa aagggagagg gagaattacc 1680 acctgtatct agaggtgctc tttgcaatcc ctaagccctc tggtcctgac ctccgacctc 1740 ccagctctgt cttgttcctt gtctttgtct ttcttccctt ccccctgccc ctgcccctac 1800 cagcccagct ttggggacac catccttctg gggagaagta gggggaggaa tatttggatg 1860 gtccctccat tcctcttcag gcatctggag gccctctccc ccactcctcc aaagaaacat 1920 ctcaaattat tgatggaatg tatccccatt ctcagtgaaa atgtgaggag gggactaata 1980 ctggggtaaa gggtcaaacc cccaccttca tcactatggg cattatattt agggagtagt 2040 tcttgggctg gattttctgg ttgtggaagt gggggcgcca gagtagtgtg tctgctattt 2100 aaaggagcag gaaagggcgt gaggcaggag gagagactgg tggagggaag agctgctcct 2160 cccatgcagt gcccgactcc ctgcacccct ctcaacctga cctgaacctt tattgaatcc 2220 ttattagctt gaatccttat tagcttgaat cctccatgca aatcatggag tctgtgtccc 2280 acctgatgtg gttgaggaga agccaggtct tcaaagaggg gtcagcctgg ggcaaagcag 2340 gactgggggg aggtgggcag cagggcctat tctgagaatc acatattgtt acaggccttg 2400 cacccccttt gctgcttccc tcctgctcat ttggggctgc caccagctct ccaccctcct 2460 ggttccgctg gccgggccaa gagaggatgg agggatggga gtcccaggag atccttgtaa 2520 atagtggggt gggactgttc tgagtgatca cccgagcact taaagctcca gagtcccatt 2580 cttcctggat ggagcaggtg gaggtgcaga ggggatttcc tcctctcctt cctcctgtcg 2640 agaattaaca cctctccaca gccttcccct ccagaacacc agccagggag gggtggggaa 2700 ggaggtcaca gccaagaaaa ctgccctgtg acgacttccc tccttcccgc ctatgtgagc 2760 catcctgaga tgtctgtaca atagaaacca aaccaaatgg gcaccctcgg ttgccggggg 2820 gcaggtgggg aggggggtgg gaagaaggga tgtctgtctg tcgtccccct ccccctctcc 2880 actctttacc cacaaaggca gaagactgtt acactagggg gctcagcaaa ttcaatccca 2940 cccttaccaa ttgagccaaa cctagaaaca aacacaaaac acgaatagtg agagacaaaa 3000 tagaggagag aaagagagca tgagagggag cgagacaggc gaccaacaca gaggagagaa 3060 aacaaaaata gc 3072 <210> SEQ ID NO 245 <211> LENGTH: 2323 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 245 ggactctggc tttgaggccc cacgcctggg tgagcagggc ggggactttg gctacggcgg 60 gtacctcttt ccgggctatg gcgtgggcaa gcaggatgtg tactacggcg tggccgagac 120 tagccccccg ctgtgggcgg gccaggagaa cgccacgccc acctccgtgc tcttctcctc 180 ctcctcctcc tcctcctctt ccgccaaggc ccgcgctggg cccccgggcg cacaccgctc 240 ccctgccact tccgcgggac ccgagctggc cggactcccg aggcgccccc cgggagagcc 300 gctccggggc ttctctaaac ttggtggggg cggcctgcgg agccccgcag ccggcgggcg 360 ggattgcatg gtctgctttg agagcgaagt gactgccgcc cttgtgccct gcggacacaa 420 cctgttctgc atggagtgtg cagtacgcat ctgcgagagg acggacccag agtgtcccgt 480 ctgccacatc acagccacgc aagccatccg aatattctcc taagccccgt gccccatgcc 540 tccggggccc actccactgg gcccaccctg gacctgtttt ccactaaagc cttttggaaa 600 gcggtgattt gaggggcaag gtgcttagag atactcgctc gctggggaag gggggaggga 660 ggcagtggtg gctggagggt gcgccacttt cagagcctct ggtcaccctg tcctggaaag 720 attgggaggg ggccagactg aaaattttac tagagttaca actctgatac ctcaacacac 780 ccttaaatct ggaagcagct aagagaaact tttgttttgc cagaggtggc cactaaggca 840 ttctgacgcc ctctgcccac ctcccccgct gtgtgtcact ccaccccttc ttccgaggag 900 ggggtgggta aaagggagag ggagaattac cacctgtatc tagaggtgct ctttgcaatc 960 cctaagccct ctggtcctga cctccgacct cccagctctg tcttgttcct tgtctttgtc 1020 tttcttccct tccccctgcc cctgccccta ccagcccagc tttggggaca ccatccttct 1080 ggggagaagt agggggagga atatttggat ggtccctcca ttcctcttca ggcatctgga 1140 ggccctctcc cccactcctc caaagaaaca tctcaaatta ttgatggaat gtatccccat 1200 tctcagtgaa aatgtgagga ggggactaat actggggtaa agggtcaaac ccccaccttc 1260 atcactatgg gcattatatt tagggagtag ttcttgggct ggattttctg gttgtggaag 1320 tgggggcgcc agagtagtgt gtctgctatt taaaggagca ggaaagggcg tgaggcagga 1380 ggagagactg gtggagggaa gagctgctcc tcccatgcag tgcccgactc cctgcacccc 1440 tctcaacctg acctgaacct ttattgaatc cttattagct tgaatcctta ttagcttgaa 1500 tcctccatgc aaatcatgga gtctgtgtcc cacctgatgt ggttgaggag aagccaggtc 1560 ttcaaagagg ggtcagcctg gggcaaagca ggactggggg gaggtgggca gcagggccta 1620 ttctgagaat cacatattgt tacaggcctt gcaccccctt tgctgcttcc ctcctgctca 1680 tttggggctg ccaccagctc tccaccctcc tggttccgct ggccgggcca agagaggatg 1740 gagggatggg agtcccagga gatccttgta aatagtgggg tgggactgtt ctgagtgatc 1800 acccgagcac ttaaagctcc agagtcccat tcttcctgga tggagcaggt ggaggtgcag 1860 aggggatttc ctcctctcct tcctcctgtc gagaattaac acctctccac agccttcccc 1920 tccagaacac cagccaggga ggggtgggga aggaggtcac agccaagaaa actgccctgt 1980 gacgacttcc ctccttcccg cctatgtgag ccatcctgag atgtctgtac aatagaaacc 2040 aaaccaaatg ggcaccctcg gttgccgggg ggcaggtggg gaggggggtg ggaagaaggg 2100 atgtctgtct gtcgtccccc tccccctctc cactctttac ccacaaaggc agaagactgt 2160 tacactaggg ggctcagcaa attcaatccc acccttacca attgagccaa acctagaaac 2220 aaacacaaaa cacgaatagt gagagacaaa atagaggaga gaaagagagc atgagaggga 2280 gcgagacagg cgaccaacac agaggagaga aaacaaaaat agc 2323 <210> SEQ ID NO 246 <211> LENGTH: 5882 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1100,1975,4288,5859,5862,5863,5868 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 246 gcgcagacgc cccagccccc caccgccccc aaaggggcga gcgacgccaa gctctgcgct 60 ctctacaaag aggccgagct gcgcctgaag ggcagcagca acaccacgga gtgtgttccc 120 gtgcccacct ccgagcacgt ggccgagatc gtgggcaggc aaggctgcaa gattaaggcc 180 ttgagggcca agaccaacac ctacatcaag acaccggtga ggggcgagga accagtgttc 240 atggtgacag ggcgacggga ggacgtggcc acagcccggc gggaaatcat ctcagcagcg 300 gagcacttct ccatgatccg tgcctcccgc aacaagtcag gcgccgcctt tggtgtggct 360 cctgctctgc ccggccaggt gaccatccgt gtgcgggtgc cctaccgcgt ggtggggctg 420 gtggtgggcc ccaaaggggc aaccatcaag cgcatccagc agcaaaccaa cacatacatt 480 atcacaccaa gccgtgaccg cgaccccgtg ttcgagatca cgggtgcccc aggcaacgtg 540 gagcgtgcgc gcgaggagat cgagacgcac atcgcggtgc gcactggcaa gatcctcgag 600 tacaacaatg aaaacgactt cctggcgggg agccccgacg cagcaatcga tagccgctac 660 tccgacgcct ggcgggtgca ccagcccggc tgcaagcccc tctccacctt ccggcagaac 720 agcctgggct gcatcggcga gtgcggagtg gactctggct ttgaggcccc acgcctgggt 780 gagcagggcg gggactttgg ctacggcggg tacctctttc cgggctatgg cgtgggcaag 840 caggatgtgt actacggcgt ggccgagact agccccccgc tgtgggcggg ccaggagaac 900 gccacgccca cctccgtgct cttctcctct gcctcctcct cctcctcctc ttccgccaag 960 gcccgcgctg ggcccccggg cgcacaccgc tcccctgcca cttccgcggg acccgagctg 1020 gccggactcc cgaggcgccc cccgggagag ccgctccagg gcttctctaa acttggtggg 1080 ggcggcctgc ggagccccgs cggcgggcgg gattgcatgg tctgctttga gagcgaagtg 1140 actgccgccc ttgtgccctg cggacacaac ctgttctgca tggagtgtgc agtacgcatc 1200 tgcgagagga cggacccaga gtgtcccgtc tgccacatca cagccacgca agccatccga 1260 atattctcct aagccccgtg ccccatgcct ccggggccca ctccactggg cccaccctgg 1320 acctgttttc cactaaagcc ttttggaaag cggtgatttg aggggcaagg tgcttagaga 1380 tactcgctcg ctggggaagg ggggagggag gcagtggtgg ctggagggtg cgccactttc 1440 agagcctctg gtcaccctgt cctggaaaga ttgggagggg gccagactga aaattttact 1500 agagttacaa ctctgatacc tcaacacacc cttaaatctg gaagcagcta agagaaactt 1560 ttgttttgcc agaggtggcc actaaggcat tctgacgccc tctgcccacc tcccccgctg 1620 tgtgtcactc caccccttct tccgaggagg gggtgggtaa aagggagagg gagaattacc 1680 acctgtatct agaggtgctc tttgcaatcc ctaagccctc tggtcctgac ctccgacctc 1740 ctaacatgac cctttacctc ccaccccacc cccatatcct gtttgggaaa ctgtcaccag 1800 tttccagcag tgtaagggag ttggagtcct atcagaagtt gcatagatct tctaggggtt 1860 ggggagagaa gcatgtcaat cgtttctgtg gctgaaaggc tcagaagcca tctgtcccca 1920 caaagctggg ctagaggaat ctggagagga gtcctcctct ctgcccctgt ccccygcagt 1980 gtttcccttc actctctccg cctatcttcc cttcctttgg gatcttccct ttcctcaact 2040 ctttcctttc cctccagctc tttgctttgc tttcttttgg tggctgtcac tcccagctct 2100 gtcttgttcc ttgtctttgt ctttcttccc ttccccctgc ccctgcccct accagcccag 2160 ctttggggac accatccttc tggggagaag tagggggagg aatatttgga tggtccctcc 2220 attcctcttc aggcatctgg aggccctctc ccccactcct ccaaagaaac atctcaaatt 2280 attgatggaa tgtatcccca ttctcagtga aaatgtgagg aggggactaa tactggggta 2340 aagggtcaaa cccccacctt catcactatg ggcattatat ttagggagta gttcttgggc 2400 tggattttct ggttgtggaa gtgggggcgc cagagtagtg tgtctgctat ttaaaggagc 2460 aggaaagggc gtgaggcagg aggagagact ggtggaggga agagctgctc ctcccatgca 2520 gtgcccgact ccctgcaccc ctctcaacct gacctgaacc tttattgaat ccttattagc 2580 ttgaatcctt attagcttga atcctccatg caaatcatgg agtctgtgtc ccacctgatg 2640 tggttgagga gaagccaggt cttcaaagag gggtcagcct ggggcaaagc aggactgggg 2700 ggaggtgggc agcagggcct attctgagaa tcacatattg ttacaggcct tgcaccccct 2760 ttgctgcttc cctcctgctc atttggggct gccaccagct ctccaccctc ctggttccgc 2820 tggccgggcc aagagaggat ggagggatgg gagtcccagg agatccttgt aaatagtggg 2880 gtgggactgt tctgagtgat cacccgagca cttaaagctc cagagtccca ttcttcctgg 2940 atggagcagg tggaggtgca gaggggattt cctcctctcc ttcctcctgt cgagaattaa 3000 cacctctcca cagccttccc ctccagaaca ccagccaggg aggggtgggg aaggaggtca 3060 cagccaagaa aactgccctg tgacgacttc cctccttccc gcctatgtga gccatcctga 3120 gatgtctgta caatagaaac caaaccaaat gggcaccctc ggttgccggg gggcaggtgg 3180 ggaggggggt gggaagaagg gatgtctgtc tgtcgtcccc ctccccctct ccactcttta 3240 cccacaaagg cagaagactg ttacactagg gggctcagca aattcaatcc cacccttacc 3300 aattgagcca aacctagaaa caaacacaaa acacgaatag tgagagacaa aatagaggag 3360 agaaagagag catgagaggg agcgagacag gcgaccaaca cagaggagag aaaacaaaaa 3420 tagcaaaaaa aaaaaaaaaa aagcagttct ttataattta atattctatt ttaataaagg 3480 cgtttattac catataaatg tagcaaagaa cctgggctaa tatgaaaaaa aaagactttt 3540 tattaggtaa tttattatat gaaaaggata ttttatttta tgataaagtg atccttaaaa 3600 aaataaaaaa actttagaag gtttagaata tatgtaggga gagaagaaga aaaaaataca 3660 tttgtattca gagttaaatc ttaaaaaaaa aaagtgtttt taatatatgt ttgggtttac 3720 gttgcttttt tcccccactt tttttttggg gaggaatgtc atttgctttt cttgggggag 3780 catcccgggg gtgaatggtg gagagaggag ctgggggaac ccggtccctc ctgggaccct 3840 tccagtagat tggatttcac tccatggact cctcctcccc tctccccctc cccctcaggg 3900 gagccggcag agccaaacaa agaaagggat taacaagaaa ggaagaagct gtaggactaa 3960 ggactgagga tcctggggtg tcccccacca ctttcccctg ccctgtcgca ggggcaagtg 4020 aggaggggga atccagaatt aaggcctagc aggcctatag gaaccctcag agatgtgtga 4080 gatttaagag atctagattt ttttttaacc aaaaacaaga gagaaagaga agaaaaagag 4140 aaaccgaggg gtttaaaaga aaagaatact acaaaataat aattattaat aataataatt 4200 caaatttatt tcatataatc ctagagagag aaagaaacaa ttactagtta cttagtagac 4260 aatattaaga tagcttaaag tttagtasca ttgagggccc ctgggtccag tagaatgtat 4320 aaaagttgta aggaaaagat aaatagagga gggaagtggc tgagtccacc ctgagttgcc 4380 caatcttcag ataccagggt tggatcaggt tgctagttta agattgggag cttccagtct 4440 gctggggttg attctgagaa tccttggatt tttaaattgt aggacaaaga aatgaggggt 4500 tcatttccca gggtcttgga aaggatgcac actgatcatc tcaataagac aggggctggg 4560 ttgggggcag cagaggaggc caagcacatt cacctgcacc cctagtacct gggcagccca 4620 tactccaatg tggtatgtcc cctcctgggg ctcccagctc aaaccctccc atgcctgctt 4680 cccccaggcc taactgagga agtccttctt gaagtgtgac ctcggtccac ttctctacag 4740 attgatttaa gagcctggga agtcattcca caaacagaca cacatgcaca cacgcttctc 4800 accttcagag cttcaagagc actgaggcga tcagtcccct acccctgttc ccatccagct 4860 ttccacttag ctttgacctc catggcagca gtagcagtaa caatctcagt aattgttctt 4920 taaagctgac tcgttcttca cctacttgca aagtgctttc ttgtctcata aaagttagat 4980 tccaagaagg acttcccacg gagtggagtg gaaacactgt ccttgaaggc ctgggagaaa 5040 ggcatcccca tgggcacaga ggctggggaa aggcacaggg actttgggtg accctaaccc 5100 tgaccctctg ctccagttca cctccatcta tatgtgttca ggtaggggtc atctactgta 5160 ccctggcctg ggaacacatt gccctcccca cacaaaactg gagggcttgg cttctgcgtg 5220 tgagaaatca acatttttaa agcacttgcc ttctaccaac cccagcttgc aatcactggg 5280 ccttcccctc ctatccaagg ggttggaggg gccccttggc tctccttttg gcaggaggag 5340 cctgcttcat tacaccaatg actctgccat ccccctccct ggccctagac cccaaacaca 5400 tctccctcta cccaatttac tcttctcgcc ccacctaggg acagattccc cctgctcttt 5460 ttgtcctaga aaccccgcta gtttgggatg gtagcgtctg gggtggggag ggcttcccct 5520 tccccactcg agggtgcggg tggggaaggg ggggtgggtg gagacagccc tggggcaggg 5580 aggatggtct ctccactgta gaaagtagag taggattgtg gtcagactta atttgaggca 5640 tctagtgaag acacgtacaa atccaccaag gaaaaagatt tcaaaagcaa aataaaagcg 5700 ggaaataaaa cagacccaag aataatcaag tcaaagtgat gttgcacaaa atgcagagaa 5760 accaagaagg gggagggtta atgtattaaa tgtgctatta agaacttaat tttattaaaa 5820 gtactattac ttaaaaaaaa aaaaaaaaaa aaaaaaaawa arwagtcrta tcgaatcgat 5880 gt 5882 <210> SEQ ID NO 247 <211> LENGTH: 343 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 247 Met Val Thr Gly Arg Arg Glu Asp Val Ala Thr Ala Arg Arg Glu Ile 5 10 15 Ile Ser Ala Ala Glu His Phe Ser Met Ile Arg Ala Ser Arg Asn Lys 20 25 30 Ser Gly Ala Ala Phe Gly Val Ala Pro Ala Leu Pro Gly Gln Val Thr 35 40 45 Ile Arg Val Arg Val Pro Tyr Arg Val Val Gly Leu Val Val Gly Pro 50 55 60 Lys Gly Ala Thr Ile Lys Arg Ile Gln Gln Gln Thr Asn Thr Tyr Ile 65 70 75 80 Ile Thr Pro Ser Arg Asp Arg Asp Pro Val Phe Glu Ile Thr Gly Ala 85 90 95 Pro Gly Asn Val Glu Arg Ala Arg Glu Glu Ile Glu Thr His Ile Ala 100 105 110 Val Arg Thr Gly Lys Ile Leu Glu Tyr Asn Asn Glu Asn Asp Phe Leu 115 120 125 Ala Gly Ser Pro Asp Ala Ala Ile Asp Ser Arg Tyr Ser Asp Ala Trp 130 135 140 Arg Val His Gln Pro Gly Cys Lys Pro Leu Ser Thr Phe Arg Gln Asn 145 150 155 160 Ser Leu Gly Cys Ile Gly Glu Cys Gly Val Asp Ser Gly Phe Glu Ala 165 170 175 Pro Arg Leu Gly Glu Gln Gly Gly Asp Phe Gly Tyr Gly Gly Tyr Leu 180 185 190 Phe Pro Gly Tyr Gly Val Gly Lys Gln Asp Val Tyr Tyr Gly Val Ala 195 200 205 Glu Thr Ser Pro Pro Leu Trp Ala Gly Gln Glu Asn Ala Thr Pro Thr 210 215 220 Ser Val Leu Phe Ser Ser Ala Ser Ser Ser Ser Ser Ser Ser Ala Lys 225 230 235 240 Ala Arg Ala Gly Pro Pro Gly Ala His Arg Ser Pro Ala Thr Ser Ala 245 250 255 Gly Pro Glu Leu Ala Gly Leu Pro Arg Arg Pro Pro Gly Glu Pro Leu 260 265 270 Gln Gly Phe Ser Lys Leu Gly Gly Gly Gly Leu Arg Ser Pro Gly Gly 275 280 285 Gly Arg Asp Cys Met Val Cys Phe Glu Ser Glu Val Thr Ala Ala Leu 290 295 300 Val Pro Cys Gly His Asn Leu Phe Cys Met Glu Cys Ala Val Arg Ile 305 310 315 320 Cys Glu Arg Thr Asp Pro Glu Cys Pro Val Cys His Ile Thr Ala Thr 325 330 335 Gln Ala Ile Arg Ile Phe Ser 340 <210> SEQ ID NO 248 <211> LENGTH: 343 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 248 Met Val Thr Gly Arg Arg Glu Asp Val Ala Thr Ala Arg Arg Glu Ile 5 10 15 Ile Ser Ala Ala Glu His Phe Ser Met Ile Arg Ala Ser Arg Asn Lys 20 25 30 Ser Gly Ala Ala Phe Gly Val Ala Pro Ala Leu Pro Gly Gln Val Thr 35 40 45 Ile Arg Val Arg Val Pro Tyr Arg Val Val Gly Leu Val Val Gly Pro 50 55 60 Lys Gly Ala Thr Ile Lys Arg Ile Gln Gln Gln Thr Asn Thr Tyr Ile 65 70 75 80 Ile Thr Pro Ser Arg Asp Arg Asp Pro Val Phe Glu Ile Thr Gly Ala 85 90 95 Pro Gly Asn Val Glu Arg Ala Arg Glu Glu Ile Glu Thr His Ile Ala 100 105 110 Val Arg Thr Gly Lys Ile Leu Glu Tyr Asn Asn Glu Asn Asp Phe Leu 115 120 125 Ala Gly Ser Pro Asp Ala Ala Ile Asp Ser Arg Tyr Ser Asp Ala Trp 130 135 140 Arg Val His Gln Pro Gly Cys Lys Pro Leu Ser Thr Phe Arg Gln Asn 145 150 155 160 Ser Leu Gly Cys Ile Gly Glu Cys Gly Val Asp Ser Gly Phe Glu Ala 165 170 175 Pro Arg Leu Gly Glu Gln Gly Gly Asp Phe Gly Tyr Gly Gly Tyr Leu 180 185 190 Phe Pro Gly Tyr Gly Val Gly Lys Gln Asp Val Tyr Tyr Gly Val Ala 195 200 205 Glu Thr Ser Pro Pro Leu Trp Ala Gly Gln Glu Asn Ala Thr Pro Thr 210 215 220 Ser Val Leu Phe Ser Ser Ala Ser Ser Ser Ser Ser Ser Ser Ala Lys 225 230 235 240 Ala Arg Ala Gly Pro Pro Gly Ala His Arg Ser Pro Ala Thr Ser Ala 245 250 255 Gly Pro Glu Leu Ala Gly Leu Pro Arg Arg Pro Pro Gly Glu Pro Leu 260 265 270 Gln Gly Phe Ser Lys Leu Gly Gly Gly Gly Leu Arg Ser Pro Gly Gly 275 280 285 Gly Arg Asp Cys Met Val Cys Phe Glu Ser Glu Val Thr Ala Ala Leu 290 295 300 Val Pro Cys Gly His Asn Leu Phe Cys Met Glu Cys Ala Val Arg Ile 305 310 315 320 Cys Glu Arg Thr Asp Pro Glu Cys Pro Val Cys His Ile Thr Ala Thr 325 330 335 Gln Ala Ile Arg Ile Phe Ser 340 <210> SEQ ID NO 249 <211> LENGTH: 343 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: variant <222> LOCATION: 287 <223> OTHER INFORMATION: Xaa = Any amino acid <400> SEQUENCE: 249 Met Val Thr Gly Arg Arg Glu Asp Val Ala Thr Ala Arg Arg Glu Ile 5 10 15 Ile Ser Ala Ala Glu His Phe Ser Met Ile Arg Ala Ser Arg Asn Lys 20 25 30 Ser Gly Ala Ala Phe Gly Val Ala Pro Ala Leu Pro Gly Gln Val Thr 35 40 45 Ile Arg Val Arg Val Pro Tyr Arg Val Val Gly Leu Val Val Gly Pro 50 55 60 Lys Gly Ala Thr Ile Lys Arg Ile Gln Gln Gln Thr Asn Thr Tyr Ile 65 70 75 80 Ile Thr Pro Ser Arg Asp Arg Asp Pro Val Phe Glu Ile Thr Gly Ala 85 90 95 Pro Gly Asn Val Glu Arg Ala Arg Glu Glu Ile Glu Thr His Ile Ala 100 105 110 Val Arg Thr Gly Lys Ile Leu Glu Tyr Asn Asn Glu Asn Asp Phe Leu 115 120 125 Ala Gly Ser Pro Asp Ala Ala Ile Asp Ser Arg Tyr Ser Asp Ala Trp 130 135 140 Arg Val His Gln Pro Gly Cys Lys Pro Leu Ser Thr Phe Arg Gln Asn 145 150 155 160 Ser Leu Gly Cys Ile Gly Glu Cys Gly Val Asp Ser Gly Phe Glu Ala 165 170 175 Pro Arg Leu Gly Glu Gln Gly Gly Asp Phe Gly Tyr Gly Gly Tyr Leu 180 185 190 Phe Pro Gly Tyr Gly Val Gly Lys Gln Asp Val Tyr Tyr Gly Val Ala 195 200 205 Glu Thr Ser Pro Pro Leu Trp Ala Gly Gln Glu Asn Ala Thr Pro Thr 210 215 220 Ser Val Leu Phe Ser Ser Ala Ser Ser Ser Ser Ser Ser Ser Ala Lys 225 230 235 240 Ala Arg Ala Gly Pro Pro Gly Ala His Arg Ser Pro Ala Thr Ser Ala 245 250 255 Gly Pro Glu Leu Ala Gly Leu Pro Arg Arg Pro Pro Gly Glu Pro Leu 260 265 270 Gln Gly Phe Ser Lys Leu Gly Gly Gly Gly Leu Arg Ser Pro Xaa Gly 275 280 285 Gly Arg Asp Cys Met Val Cys Phe Glu Ser Glu Val Thr Ala Ala Leu 290 295 300 Val Pro Cys Gly His Asn Leu Phe Cys Met Glu Cys Ala Val Arg Ile 305 310 315 320 Cys Glu Arg Thr Asp Pro Glu Cys Pro Val Cys His Ile Thr Ala Thr 325 330 335 Gln Ala Ile Arg Ile Phe Ser 340 <210> SEQ ID NO 250 <211> LENGTH: 7993 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 250 aaaaatgttt tcctttatat ttctgaggtg aaattcttcc ataggcattt caggaggttt 60 tttgtcaaac attttaaaag caaaattgat accatgtttc tataaaatac gatatgcgaa 120 atgatgccta ttgctatttg ctactgggct ggaagttagg aaatagtgac ggaaaaaccc 180 caaatgcata cagagatcat gagtacagcc agtgatgcca gtgatgtatt acgaagatta 240 caaaaaaggc cacaaaagtt caatgctaat cccttctggg tcgaacacag agtgacacat 300 tcggcagaca attatatttt acttatgtaa cgaataagtc atatttttct gtactgggca 360 tttttagagg aacatataaa gaaatggata gtgtcttagg ggtctcattt tctaatttag 420 aaatgttttc actcccatgt gaaaagattt gctaatatat aacagacaat ctaacttggg 480 gcatcctatt aaaataatct attttccata acttcaacct ttttaaaaaa taaagtcagt 540 gggaatttct aatttccctg tgggttttat ctatatgcat tttttaggtt ttttttttcc 600 ttatcatata ccttccagat tttatgttta aataaataaa tgatatttca agataaagtt 660 agtctataaa gggacactaa atcagcctac agatgtcaat ctctaggttt aactacagag 720 atagttccac ataaatgcca aaaagaagtg gttttgatgt caatctttat gaaaatggtt 780 ttatttaacc attgtatcaa gtctaactat acttgggcag atttgagctt taaaaataaa 840 gctatgtatt tcgtttttaa aaatgtgctt ctctgtttct tcatttactt acaactgtgg 900 aacagaatca cgagtttgtg gacgaacaag tctttgaaga aagctgcatg gaagttgcaa 960 ctgttaatcg tccttcaagt cacagtcctt cactgtcttc acaacaagga gtcaccagca 1020 cctgctgttc acgacgacac aaaaaaactt ttcgcatccc aaatgccaat gtatcaggaa 1080 gccatcaagg tagtatacaa gaactcagca cgattcagat cagatgtgtg gagagaacac 1140 ctctgtctaa caggtacctg agattaatct gtgttgtcta cacacctgtg ctggttccca 1200 gggtgtgtct tctgcactca tgttgtcact tacatggcat ctaaatccct agctcctatg 1260 gttcaggaag agacaaaaat ggtagcgtaa caagtaggaa aatggttctg cttgcatatc 1320 cattaagggt taaaaatagt ggttatatca gtattaaaag agtcgaaaga agaagagatg 1380 attgagtgca cacaaatgtg tttttctctc ttctgttcca caaccttttc ttatttgggc 1440 aaggactttt atactcagga gtctcttata tattcaatag tctgaaatga tggtggacac 1500 tactaaaaga gtcaaatgaa attgagatca acatggctaa aaattattga acagcatgta 1560 aaaatataca aacacactgt ctgtaacagt aaaaatgaaa actttgccta cataagtcat 1620 ttctatcaat atataatttt gatcagaaag gtatttttgg ccatatcaaa cacaaaatca 1680 acataataca aaaaataagt gaagtactaa aattgtttgc ctctggttag tttatgaaca 1740 aattaagtaa aacttccata ttgatatatt tcctttgctt ttccttattc actgttttta 1800 ccacaaatgt gtaaaaataa aaagttgtac atttaaacaa tatatgtcat taaaaatcag 1860 tttctgccaa aataatttta ttctgttttc aaattgaaca gcatatattg ttagagtgag 1920 agtctgtaaa ttcagtcctc ttctttgttg gcattcagaa gtctttgttg aaatctggat 1980 gagattctga attcaggtga tgttgattta cataaattgg atgtctctgg gactagaaaa 2040 ttaaaattag gagccataag acttctatct tcaagatatt ttagctttgc agttttatat 2100 cctttataaa gtgaagtcga caatggaaaa ttatctagca agaaaatctt aggacataaa 2160 catcttaatt atgttttcca tgaaaataaa ataatcagtt tcaagcttct gtgtatatcc 2220 ttctctctca tttccctttt atccccttcc ccacatagag tatacaattc atccaataat 2280 accatttggg agcttgaagt gttagatagt aatagataat ttttttattt ctgtaatatg 2340 tgatcatcat taagttcaga ggtttgaggg cattatatat cccaaaaaga catgaaaata 2400 aaaatattct gtggtcaaag gaattaagaa atcaatgtga tatggctctt tcatagtggt 2460 ttctcaaacc tctcagaggt ctgtcttaaa taaaacttct ttgctcagcc caggctgtcc 2520 aaatcttact tgaagctctt tctttcttac atttttttat aatacattta gtttgataaa 2580 tacttgatgg aaccaagtca aactgtcttt tagaaattta tttaatgtta attactatgt 2640 tcatctttaa catagattaa gatttggtgt ttcatatttt taattataat aactttcctt 2700 agacaattaa aatattttta taagcattac aacacatatt cttcagttgt atgaaaaaca 2760 ttttaagtaa acaacttact ttcctaaata tttttttttc tatcagccga tccagtttaa 2820 atgccaaaat ggaagagtgt gttaaactaa actgtgaaca accttatgtg actacagcaa 2880 taataagcat cccaacacct ccagtaacca caccagaagg agacgatagg ccagaatccc 2940 ctgagtactc aggaggaaat attgtcagag tttctgcttt gtaagacaat tggaataagg 3000 tctaagagaa ttcgagccct ggctgtgaaa agaatctcaa catagaagaa agaagaaaca 3060 ataaatattc tgcagattaa tgcagcaaag aaagaaggtt ggtagtgaaa cacaaagctt 3120 ccaatcttaa ggatgtgaat aaaaccacca aatggcattt ctagacagtt tgacctgtta 3180 tacagagtaa tattctgtgg ccctttgact ttgtgaatga gcacaatgaa atgccgccta 3240 ctgatgcttc ttatgatcag aactcttttt taataaaata aataacataa atcgttgaac 3300 ataatgttcc agttgaatgc aaaacaaaaa aaatatggaa aacattttga taaaattttt 3360 tcctgttaaa accatgaaca ttggctatga tgaagattat tacatatgaa aaaaaaactc 3420 acacaacata tttgtattga ctgaaggaaa ccatcataat gcatgctaga attctttgaa 3480 gcagtgatct cagtttcctt atgttgtctt cagaataggc atgataaact ataattgtag 3540 aaaggggtaa tttctgtgca cttacaacaa gctgagtgtt catgttccat ggtgggctgt 3600 gcaaataaac tccttttaga cctgcagtat ttctcatggg gatgctcatt agtaaatcta 3660 aagtgttcag atagttcagt attcattatc gtttaacttt gcacctagat actgttacaa 3720 ctgcaataat ttgttgtaca actgttgtat caggaatcag gatttttttg ttgttgtact 3780 ttccagatcc ttatagatac ggtaagagcc acattcgtag aaaaacttct ggtgtggcca 3840 ggttttaggt aactttttaa tccaaaacta ttgtgccata aatgtttttc agtaatattt 3900 tttggtccac tgtattcctg tgacacagtg cattatctgt tcttgtattt ctatagcacc 3960 tctctattgg gtttatcatc atcaacaaga ctactgttta ctgtagttca agtgactttc 4020 ctacttttgt atttccaaaa aaaattatct tgtaagtagc ttgtcatcaa tccccttgtc 4080 gaaaactaga aaaaaaggag ttgacccata taaattatct ctaacgtctt tgttgtttat 4140 ggaaaagccc agatactgga tatatcacta tgtattttat gaacagaatt gactgggact 4200 aatatcacag gatcaatcat ctcagaatct tacttgatgc attatttatt ttgctttaga 4260 tcttgaatac attttgagaa taactaatgt ggattgaaat gtagagatac actggagtgc 4320 tttatttagc aatatttgat gaaagcatgc tttctacgcc attcaggaag gcagcacaaa 4380 tttatctcag aaaggttcct gtgtattgca aggtacaatt ttctccaata aatcaggaga 4440 acaggagttt gatgatgcaa agttgatctc tgtacattta agtgaaaagt ctttataact 4500 tttcaccctt aaaatatttc agcagacatg tctgcacatg acagtgtaaa aaagtttaat 4560 gtcaaatgca aagtttttat tcattccaag ccaccactgt aaggaataaa gcttagcttc 4620 tgtacatgga aagagctaat aattatccct ctgtcagaga tgagattttt aaatgcttat 4680 gatatttaat cataaaaagg gattaatcca accattttct agtaaagcca gaaattcttg 4740 cttcccattt ctagaatagt ttctagaaca gtgctatgca catattagat cttaataaac 4800 atttgctgag tgaaagtaag ataaactcaa ctatctcttg ggaagaactg gcttcattcc 4860 tagtacatct tttaaaaagt tactaatttt ccagcagtac aaatattaac aattatatta 4920 acacctgcct catgtcagtt tatgcttcta gagcaatgtc tagtgaaact tatctgatgg 4980 catttattga aaaccttcta aaaagtagac taaggaaacc ataatcagaa ttactatgtc 5040 ttttgattcc caatgagaag ttctattttc atgttcttaa tattacatac aagaaaatgc 5100 agttaggtta tttcaattga caattctgcc tcctcttttg atttatcact tacccaaaat 5160 tattaatttt attaggcttt tggaaaagaa aaaaaacttt ttgatgtttt aggtgattta 5220 aaaatatacc gtgttggtgg tgaatgacta ttgatgactg tgttaagtgc atctgtattg 5280 taagtgaaat gtaattattt ctgtgtacca tatggagtaa ctaaggtcat tgtttttgac 5340 aattttgttt gaaattcata tatcttattt caaaggatag cataatatct gcattatgct 5400 ggaaaaaaat agacctttgg agaatactta aataaaacat gtgcatgctt gaacaggaca 5460 aaatgttgac tgttgcccta ttttcttaga tttcattcct ttcccaaaat taggatatgc 5520 cacactcata atacacatgt tggaggacct tgtgagacat acaactcaaa ggacacagca 5580 attgaaagta atgcttaaat ctcatctgaa tgggtggaga cagtagcttt tgctagtaat 5640 gggaattaag gcagggactt taacagaaaa gatagtatca attaaggaaa gccagtccct 5700 gaaccttata tacttcttaa acaccactac ttgcattaag cagagaagct caggggtaat 5760 ggttttggtc agaacttaaa taaattctta atcaaaggct ttattctacc taggaaagcg 5820 gggtgattta tttgcctagc catttgtgtg catgtatgtg tatatgtaga tataaatttg 5880 ttcatacaca tatacataga ttttcattca tttttaatat gcaaccacta atggtttctc 5940 ttaatatctt gaaagggcta aaaagcaaga aaatgttaag agtttataga agaaggaaaa 6000 agacacaaag gaaattattt agtagaaaga ctgattttaa ctggtgatat atatggtcct 6060 cttggtggat agtctctatc ttttcttgtt aattattttc atttatagcc tttgatttat 6120 taggtatcaa tcttgcatta aaaagttcaa tatgcctccc tattccttca acttagtcac 6180 aatgttggct tagaaatagc ctcttgggag ctataatgtg tctgccagta acattgctca 6240 aaagaataaa aaagggttct tgaaagtaaa ttgataactc cttagagttt cataagaaag 6300 gcatcttctc ttccctacag tgtcattaag gtgtttgttt tattaactca ctggtacaag 6360 aatggttatt actctgcact gtgtaaacat ctgaattttc aacacaattg tgtaggcaca 6420 cagtattttt ttaatgaagg tttaaattgt acctacgaag gtttaagtct tatctacttc 6480 agctggttgt attaggatac taaaatattc tttacagagt ttgatttttt acttctaagg 6540 aattactagc tttgaacagc aagtttgctt aagataatta taaaatataa ttttacaaaa 6600 tatttttagt tgaaaataat attaaataca tagcatacct ttaatctttc tctttactgc 6660 ctgccctgcc ttttttctcc tttatcttca agcattaatt attattgtag cagatctttg 6720 cctttcccta attacttttt tctctagctt ttctatggaa atcctttagg ttacataact 6780 aatattcatt ctacatataa tccagtttat taaatacaga tgatgggcca gacatggtga 6840 tagagaaata cagattaaga aaccagatca aatccttttt aaggaattat ctagtggaaa 6900 atatctcaac tctcttcttt acactactat tcattatctt acacttcaaa tcttcacctt 6960 tccattttga cagtcgctct tctacttcag tctcctgaag acatctctcc aacagaagtt 7020 acataaaaat actaatcttc aaggtgcttt ctaaaatatt ttcatcacgt cattaaaatc 7080 ttctttcact aggcaatggt tctgtctcta tgggggctgg caggcagggc aaatgaattc 7140 ctacctgccc agagaaagaa caggaaacaa taaaggtaaa acaaaaccca aaggaagaag 7200 agcttcatgt ttatgcatta cattaaagtt aaaaggaaat aaactttctc aagtatccac 7260 tctacctttt caactataat ttcagagaat gtgaagaaag ctattaaaat agttttgcag 7320 gaggactgat acacaatgcg tctgtgaatc tgaacaccac acctcaaatt ctattatctg 7380 atgaatccta ttgaaatatc tgagtaattg ggacaacaga aaggtaagtc tgtaatcagg 7440 ggcactcacc aataaggcgg gcctagttgg ttcatgtcaa ttccaaagca agaggatggt 7500 tgaagaaggg tattgaatga gtagataaca aatatttgga gagagatttg gaggaaccct 7560 ggaagacaag agtaggctat tggcaagggc tacaagatgg tagagacatc cttgggcttt 7620 gactctaatt gaaaatacag aattttggcc tgacgcagtg actcatgcct gtaatcctag 7680 cactttggga ggctgagggg ggtggatcac ttgaggtcag gagtccaaga ccagcctcat 7740 caactggtga aaccccatct ctactaaaaa aagaaaaaaa aaaaatagcc aggtgtcctg 7800 gtgcatgcct gtaatctcag ctactcagga gtctgaggca ggagaattgc ttgaactcgg 7860 gaggtggagg ttgcaatgag ctgagattgt gccactgcat tccagcctgg gtgacagggg 7920 gagactccgt cttaaaaaaa gaaaaaagaa aaaccagaat tttaaagttc aatttagatc 7980 aaattaattc ctt 7993 <210> SEQ ID NO 251 <211> LENGTH: 3254 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 251 ggtatggtga catggtgcca aaaaccatag cagggaagat ttttggttct atctgttcgc 60 tgagtggggt cttggtcatt gctctacctg ttccggtgat tgtatccaac ttcagtcgca 120 tctaccacca gaatcaacga gcagacaaac gaagggcaca aaagaaagct agactggcca 180 ggatccgggc agccaaaagc ggaagcgcaa atgcttacat gcagagcaaa cggaatggtt 240 tactcagtaa tcagctgcag tcctcagagg atgagcaggc ttttgttagc aaatccggct 300 ccagctttga aacccagcac caccacctgc ttcactgcct ggaaaaaacc acgaatcacg 360 agtttgtgga cgaacaagtc tttgaagaaa gctgcatgga agttgcaact gttaatcgtc 420 cttcaagtca cagtccttca ctgtcttcac aacaaggagt caccagcacc tgctgttcac 480 gacgacacaa aaaaactttt cgcatcccaa atgccaatgt atcaggaagc catcaaggta 540 gtatacaaga actcagcacg attcagatca gatgtgtgga gagaacacct ctgtctaaca 600 gccgatccag tttaaatgcc aaaatggaag agtgtgttaa actaaactgt gaacaacctt 660 atgtgactac agcaataata agcatcccaa cacctccagt aaccacacca gaaggagacg 720 ataggccaga atcccctgag tactcaggag gaaatattgt cagagtttct gctttgtaag 780 acaattggaa taaggtctaa gagaattcga gccctggctg tgaaaagaat ctcaacatag 840 aagaaagaag aaacaataaa tattctgcag attaatgcag caaagaaaga aggttggtag 900 tgaaacacaa agcttccaat cttaaggatg tgaataaaac caccaaatgg catttctaga 960 cagtttgacc tgttatacag agtaatattc tgtggccctt tgactttgtg aatgagcaca 1020 atgaaatgcc gcctactgat gcttcttatg atcagaactc ttttttaata aaataaataa 1080 cataaatcgt tgaacataat gttccagttg aatgcaaaac aaaaaaaata tggaaaacat 1140 tttgataaaa ttttttcctg ttaaaaccat gaacattggc tatgatgaag attattacat 1200 atgaaaaaaa aactcacaca acatatttgt attgactgaa ggaaaccatc ataatgcatg 1260 ctagaattct ttgaagcagt gatctcagtt tccttatgtt gtcttcagaa taggcatgat 1320 aaactataat tgtagaaagg ggtaatttct gtgcacttac aacaagctga gtgttcatgt 1380 tccatggtgg gctgtgcaaa taaactcctt ttagacctgc agtatttctc atggggatgc 1440 tcattagtaa atctaaagtg ttcagatagt tcagtattca ttatcgttta actttgcacc 1500 tagatactgt tacaactgca ataatttgtt gtacaactgt tgtatcagga atcaggattt 1560 ttttgttgtt gtactttcca gatccttata gatacggtaa gagccacatt cgtagaaaaa 1620 cttctggtgt ggccaggttt taggtaactt tttaatccaa aactattgtg ccataaatgt 1680 ttttcagtaa tattttttgg tccactgtat tcctgtgaca cagtgcatta tctgttcttg 1740 tatttctata gcacctctct attgggttta tcatcatcaa caagactact gtttactgta 1800 gttcaagtga ctttcctact tttgtatttc caaaaaaaat tatcttgtaa gtagcttgtc 1860 atcaatcccc ttgtcgaaaa ctagaaaaaa aggagttgac ccatataaat tatctctaac 1920 gtctttgttg tttatggaaa agcccagata ctggatatat cactatgtat tttatgaaca 1980 gaattgactg ggactaatat cacaggatca atcatctcag aatcttactt gatgcattat 2040 ttattttgct ttagatcttg aatacatttt gagaataact aatgtggatt gaaatgtaga 2100 gatacactgg agtgctttat ttagcaatat ttgatgaaag catgctttct acgccattca 2160 ggaaggcagc acaaatttat ctcagaaagg ttcctgtgta ttgcaaggta caattttctc 2220 caataaatca ggagaacagg agtttgatga tgcaaagttg atctctgtac atttaagtga 2280 aaagtcttta taacttttca cccttaaaat atttcagcag acatgtctgc acatgacagt 2340 gtaaaaaagt ttaatgtcaa atgcaaagtt tttattcatt ccaagccacc actgtaagga 2400 ataaagctta gcttctgtac atggaaagag ctaataatta tccctctgtc agagatgaga 2460 tttttaaatg cttatgatat ttaatcataa aaagggatta atccaaccat tttctagtaa 2520 agccagaaat tcttgcttcc catttctaga atagtttcta gaacagtgct atgcacatat 2580 tagatcttaa taaacatttg ctgagtgaaa gtaagataaa ctcaactatc tcttgggaag 2640 aactggcttc attcctagta catcttttaa aaagttacta attttccagc agtacaaata 2700 ttaacaatta tattaacacc tgcctcatgt cagtttatgc ttctagagca atgtctagtg 2760 aaacttatct gatggcattt attgaaaacc ttctaaaaag tagactaagg aaaccataat 2820 cagaattact atgtcttttg attcccaatg agaagttcta ttttcatgtt cttaatatta 2880 catacaagaa aatgcagtta ggttatttca attgacaatt ctgcctcctc ttttgattta 2940 tcacttaccc aaaattatta attttattag gcttttggaa aagaaaaaaa actttttgat 3000 gttttaggtg atttaaaaat ataccgtgtt ggtggtgaat gactattgat gactgtgtta 3060 agtgcatctg tattgtaagt gaaatgtaat tatttctgtg taccatatgg agtaactaag 3120 gtcattgttt ttgacaattt tgtttgaaat tcatatatct tatttcaaag gatagcataa 3180 tatctgcatt atgctggaaa aaaatagacc tttggagaat acttaaataa aacatgtgca 3240 tgcttgaaca ggac 3254 <210> SEQ ID NO 252 <211> LENGTH: 5333 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 252 cggctgctcg cgagctgctt tctctcctct tccctttccg ggtgcacggc gaggagaaag 60 tctctatgca actaagcccc ggcgcgcact tggccaggta tgtaccgcgg gagcggcgcg 120 ttctgcgcgg aagcagatgc tgctgccgcc acggcggcgg cggctgccag ctcctgagct 180 ctgtaactgt cacactgcac ctgagctgaa cttgaaaaga gagtgaaggg gcgattgggc 240 gaacgctttt ggcagacaca gagggtgttt gtagacgtgg gggaggagaa tctctattaa 300 cgccccccac cgtaaccact gcacatcacc tccatctctg caaatacagc ccgaggagta 360 gaggcagcag cagctggacc cccaaagaga gacgtggggc agcggctgtg accgcatctc 420 ctgagctaca acaacaggtc gcctttttga gactcctttg gcgggaaggg ctacttggaa 480 aggaaggttt gaaagagtga gaagggtagg tgtaagggtt ccctaattcg tcgaaagaat 540 tctattgggt gactctcgtt cgtcttctct atcctacact ccacatactg accctatatt 600 atccagactg tgccggggag aaatcaaaaa cacctgtttg aagaaacggc tgcacctgtg 660 tgcttatttg tgccagaggg tggcctagcc cacctgcagg aagagatttg gctgggttct 720 gttgagggtg attgttagga cgttgtattt tgttgccatt attccaaata cctgtcttgg 780 agggaaagtt gcccttctga gaactgtgac tttaccagga gccctatctt ggaataagag 840 ttacacctct ggaccacgtt tctcactagt actttgcttg actggaggaa gtgggtgact 900 tttggctgct tcggtgaccc attgtagacg cctcgttacc cttcttcctt ccgcttcaag 960 taatcatggc ggcgggggtg gcagcgtggc tgccttttgc aagggcagcg gctatcgggt 1020 ggatgcctgt ggcctcgggg cctatgccgg ctcccccgag gcaggagagg aaaaggaccc 1080 aagatgctct cattgtgctg aatgtgagtg gcacccgctt ccagacgtgg caggacaccc 1140 tggaacgtta cccagacact ctactgggca gttctgagag ggactttttc taccacccag 1200 aaactcagca gtatttcttt gaccgtgacc cagacatctt ccgccacatc ctgaatttct 1260 accgcactgg gaagctccac tatcctcgcc acgagtgcat ctctgcttac gatgaagaac 1320 tggccttctt tggcctcatc ccggaaatca tcggcgactg ctgttatgag gagtacaagg 1380 atcgcaggcg agagaacgcc gagcgcctgc aggacgacgc ggataccgac accgctgggg 1440 agagcgcctt gcccaccatg actgcaaggc agagggtctg gagggccttc gagaaccccc 1500 acaccagcac gatggccctg gtgttctact atgtcacggg gtttttcatt gccgtctctg 1560 tcatcgcgaa tgtggtggaa acagtgccgt gcggatcaag cccaggtcac attaaagaac 1620 tgccctgtgg agagcggtat gctgtggcct tcttctgctt ggacacggcc tgcgtcatga 1680 tcttcacagt tgagtatttg cttcgcctgg ctgcagcgcc tagtcgttac cgttttgtgc 1740 gtagtgtcat gagtatcatc gacgtggtgg ccatcctgcc ttattacatt gggctggtga 1800 tgacagacaa tgaggacgtc agcggagcct ttgtcacact ccgagtcttc cgggtcttca 1860 ggatctttaa gttttcccgc cactctcaag gcctgcgcat cctggggtac acactgaaga 1920 gttgtgcctc agaattgggc ttcttgcttt tctcgctcac catggctatc atcatcttcg 1980 ctacagttat gttctacgca gagaaggggt cttcggctag caagttcacc agcatccctg 2040 cagccttctg gtataccatc gtcaccatga caacactagg gtatggtgac atggtgccaa 2100 aaaccatagc agggaagatt tttggttcta tctgttcgct gagtggggtc ttggtcattg 2160 ctctacctgt tccggtgatt gtatccaact tcagtcgcat ctaccaccag aatcaacgag 2220 cagacaaacg aagggcacaa aagaaagcta gactggccag gatccgggca gccaaaagcg 2280 gaagcgcaaa tgcttacatg cagagcaaac ggaatggttt actcagtaat cagctgcagt 2340 cctcagagga tgagcaggct tttgttagca aatccggctc cagctttgaa acccagcacc 2400 accacctgct tcactgcctg gaaaaaacca cgaatcacga gtttgtggac gaacaagtct 2460 ttgaagaaag ctgcatggaa gttgcaactg ttaatcgtcc ttcaagtcac agtccttcac 2520 tgtcttcaca acaaggagtc accagcacct gctgttcacg acgacacaaa aaaacttttc 2580 gcatcccaaa tgccaatgta tcaggaagcc atcaaggtag tatacaagaa ctcagcacga 2640 ttcagatcag atgtgtggag agaacacctc tgtctaacag ccgatccagt ttaaatgcca 2700 aaatggaaga gtgtgttaaa ctaaactgtg aacaacctta tgtgactaca gcaataataa 2760 gcatcccaac acctccagta accacaccag aaggagacga taggccagaa tcccctgagt 2820 actcaggagg aaatattgtc agagtttctg ctttgtaaga caattggaat aaggtctaag 2880 agaattcgag ccctggctgt gaaaagaatc tcaacataga agaaagaaga aacaataaat 2940 attctgcaga ttaatgcagc aaagaaagaa ggttggtagt gaaacacaaa gcttccaatc 3000 ttaaggatgt gaataaaacc accaaatggc atttctagac agtttgacct gttatacaga 3060 gtaatattct gtggcccttt gactttgtga atgagcacaa tgaaatgccg cctactgatg 3120 cttcttatga tcagaactct tttttaataa aataaataac ataaatcgtt gaacataatg 3180 ttccagttga atgcaaaaca aaaaaaatat ggaaaacatt ttgataaaat tttttcctgt 3240 taaaaccatg aacattggct atgatgaaga ttattacata tgaaaaaaaa actcacacaa 3300 catatttgta ttgactgaag gaaaccatca taatgcatgc tagaattctt tgaagcagtg 3360 atctcagttt ccttatgttg tcttcagaat aggcatgata aactataatt gtagaaaggg 3420 gtaatttctg tgcacttaca acaagctgag tgttcatgtt ccatggtggg ctgtgcaaat 3480 aaactccttt tagacctgca gtatttctca tggggatgct cattagtaaa tctaaagtgt 3540 tcagatagtt cagtattcat tatcgtttaa ctttgcacct agatactgtt acaactgcaa 3600 taatttgttg tacaactgtt gtatcaggaa tcaggatttt tttgttgttg tactttccag 3660 atccttatag atacggtaag agccacattc gtagaaaaac ttctggtgtg gccaggtttt 3720 aggtaacttt ttaatccaaa actattgtgc cataaatgtt tttcagtaat attttttggt 3780 ccactgtatt cctgtgacac agtgcattat ctgttcttgt atttctatag cacctctcta 3840 ttgggtttat catcatcaac aagactactg tttactgtag ttcaagtgac tttcctactt 3900 ttgtatttcc aaaaaaaatt atcttgtaag tagcttgtca tcaatcccct tgtcgaaaac 3960 tagaaaaaaa ggagttgacc catataaatt atctctaacg tctttgttgt ttatggaaaa 4020 gcccagatac tggatatatc actatgtatt ttatgaacag aattgactgg gactaatatc 4080 acaggatcaa tcatctcaga atcttacttg atgcattatt tattttgctt tagatcttga 4140 atacattttg agaataacta atgtggattg aaatgtagag atacactgga gtgctttatt 4200 tagcaatatt tgatgaaagc atgctttcta cgccattcag gaaggcagca caaatttatc 4260 tcagaaaggt tcctgtgtat tgcaaggtac aattttctcc aataaatcag gagaacagga 4320 gtttgatgat gcaaagttga tctctgtaca tttaagtgaa aagtctttat aacttttcac 4380 ccttaaaata tttcagcaga catgtctgca catgacagtg taaaaaagtt taatgtcaaa 4440 tgcaaagttt ttattcattc caagccacca ctgtaaggaa taaagcttag cttctgtaca 4500 tggaaagagc taataattat ccctctgtca gagatgagat ttttaaatgc ttatgatatt 4560 taatcataaa aagggattaa tccaaccatt ttcaagtaaa gccagaaatt cttgcttccc 4620 atttctagaa tagtttctag aacagtgcta tgcacatatt agatcttaat aaacatttgc 4680 tgagtgaaag taagataaac tcaactatct cttgggaaga actggcttca ttcctagtac 4740 atcttttaaa aagttactaa ttttccagca gtacaaatat taacaattat attaacacct 4800 gcctcatgtc agtttatgct tctagagcaa tgtctagtga aacttatctg atggcattta 4860 ttgaaaacct tctaaaaagt agactaagga aaccataatc agaattacta tgtcttttga 4920 ttcccaatga gaagttctat tttcatgttc ttaatattac atacaagaaa atgcagttag 4980 gttatttcaa ttgacaattc tgcctcctct tttgatttat cacttaccca aaattattaa 5040 ttttattagg cttttggaaa agaaaaaaaa ctttttgatg ttttaggtga tttaaaaata 5100 taccgtgttg gtggtgaatg actattgatg actgtgttaa gtgcatctgt attgtaagtg 5160 aaatgtaatt atttctgtgt accatatgga gtaactaagg tcattgtttt tgacaatttt 5220 gtttgaaatt catatatctt atttcaaagg atagcataat atctgcatta tgctggaaaa 5280 aaatagacct ttggagaata cttaaataaa acatgtgcat gcttgaacag gac 5333 <210> SEQ ID NO 253 <211> LENGTH: 2351 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 253 gaattctatt gggtgactct cgttcgtctt ctctatccta cactccacat actgacccta 60 tattatccag actgtgccgg ggagaaatca aaaacacctg tttgaagaaa cggctgcacc 120 tgtgtgctta tttgtgccag agggtggcct agcccacctg caggaagaga tttggctggg 180 ttctgttgag ggtgattgtt aggacgttgt attttgttgc cattattcca aatacctgtc 240 ttggagggaa agttgccctt ctgagaactg tgactttacc aggagcccta tcttggaata 300 agagttacac ctctggacca cgtttctcac tagtactttg cttgactgga ggaagtgggt 360 gacttttggc tgcttcggtg acccattgta gacgcctcgt tacccttctt ccttccgctt 420 caagtaatca tggcggcggg ggtggcagcg tggctgcctt ttgcaagggc agcggctatc 480 gggtggatgc ctgtggcctc ggggcctatg ccggctcccc cgaggcagga gaggaaaagg 540 acccaagatg ctctcattgt gctgaatgtg agtggcaccc gcttccagac gtggcaggac 600 accctggaac gttacccaga cactctactg ggcagttctg agagggactt tttctaccac 660 ccagaaactc agcagtattt ctttgaccgt gacccagaca tcttccgcca catcctgaat 720 ttctaccgca ctgggaagct ccactatcct cgccacgagt gcatctctgc ttacgatgaa 780 gaactggcct tctttggcct catcccggaa atcatcggcg actgctgtta tgaggagtac 840 aaggatcgca ggcgagagaa cgccgagcgc ctgcaggacg acgcggatac cgacaccgct 900 ggggagagcg ccttgcccac catgactgca aggcagaggg tctggagggc cttcgagaac 960 ccccacacca gcacgatggc cctggtgttc tactatgtca cggggttttt cattgccgtc 1020 tctgtcatcg cgaatgtggt ggaaacagtg ccgtgcggat caagcccagg tcacattaaa 1080 gaactgccct gtggagagcg gtatgctgtg gccttcttct gcttggacac ggcctgcgtc 1140 atgatcttca cagttgagta tttgcttcgc ctggctgcag cgcctagtcg ttaccgtttt 1200 gtgcgtagtg tcatgagtat catcgacgtg gtggccatcc tgccttatta cattgggctg 1260 gtgatgacag acaatgagga cgtcagcgga gcctttgtca cactccgagt cttccgggtc 1320 ttcaggatct ttaagttttc ccgccactct caaggcctgc gcatcctggg gtacacactg 1380 aagagttgtg cctcagaatt gggcttcttg cttttctcgc tcaccatggc tatcatcatc 1440 ttcgctacag ttatgttcta cgcagagaag gggtcttcgg ctagcaagtt caccagcatc 1500 cctgcagcct tctggtatac catcgtcacc atgacaacac tagggtatgg tgacatggtg 1560 ccaaaaacca tagcagggaa gatttttggt tctatctgtt cgctgagtgg ggtcttggtc 1620 attgctctac ctgttccggt gattgtatcc aacttcagtc gcatctacca ccagaatcaa 1680 cgagcagaca aacgaagggc acaaaagaaa gctagactgg ccaggatccg ggcagccaaa 1740 agcggaagcg caaatgctta catgcagagc aaacggaatg gtttactcag taatcagctg 1800 cagtcctcag aggatgagca ggcttttgtt agcaaatccg gctccagctt tgaaacccag 1860 caccaccacc tgcttcactg cctggaaaaa accacgaatc acgagtttgt ggacgaacaa 1920 gtctttgaag aaagctgcat ggaagttgca actgttaatc gtccttcaag tcacagtcct 1980 tcactgtctt cacaacaagg agtcaccagc acctgctgtt cacgacgaca caaaaaaact 2040 tttcgcatcc caaatgccaa tgtatcagga agccatcaag gtagtataca agaactcagc 2100 acgattcaga tcagatgtgt ggagagaaca cctctgtcta acagccgatc cagtttaaat 2160 gccaaaatgg aagagtgtgt taaactaaac tgtgaacaac cttatgtgac tacagcaata 2220 ataagcatcc caacacctcc agtaaccaca ccagaaggag acgataggcc agaatcccct 2280 gagtactcag gaggaaatat tgtcagagtt tctgctttgt aagacaattg gaataaggtc 2340 taagagaatt c 2351 <210> SEQ ID NO 254 <211> LENGTH: 5333 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 254 cggctgctcg cgagctgctt tctctcctct tccctttccg ggtgcacggc gaggagaaag 60 tctctatgca actaagcccc ggcgcgcact tggccaggta tgtaccgcgg gagcggcgcg 120 ttctgcgcgg aagcagatgc tgctgccgcc acggcggcgg cggctgccag ctcctgagct 180 ctgtaactgt cacactgcac ctgagctgaa cttgaaaaga gagtgaaggg gcgattgggc 240 gaacgctttt ggcagacaca gagggtgttt gtagacgtgg gggaggagaa tctctattaa 300 cgccccccac cgtaaccact gcacatcacc tccatctctg caaatacagc ccgaggagta 360 gaggcagcag cagctggacc cccaaagaga gacgtggggc agcggctgtg accgcatctc 420 ctgagctaca acaacaggtc gcctttttga gactcctttg gcgggaaggg ctacttggaa 480 aggaaggttt gaaagagtga gaagggtagg tgtaagggtt ccctaattcg tcgaaagaat 540 tctattgggt gactctcgtt cgtcttctct atcctacact ccacatactg accctatatt 600 atccagactg tgccggggag aaatcaaaaa cacctgtttg aagaaacggc tgcacctgtg 660 tgcttatttg tgccagaggg tggcctagcc cacctgcagg aagagatttg gctgggttct 720 gttgagggtg attgttagga cgttgtattt tgttgccatt attccaaata cctgtcttgg 780 agggaaagtt gcccttctga gaactgtgac tttaccagga gccctatctt ggaataagag 840 ttacacctct ggaccacgtt tctcactagt actttgcttg actggaggaa gtgggtgact 900 tttggctgct tcggtgaccc attgtagacg cctcgttacc cttcttcctt ccgcttcaag 960 taatcatggc ggcgggggtg gcagcgtggc tgccttttgc aagggcagcg gctatcgggt 1020 ggatgcctgt ggcctcgggg cctatgccgg ctcccccgag gcaggagagg aaaaggaccc 1080 aagatgctct cattgtgctg aatgtgagtg gcacccgctt ccagacgtgg caggacaccc 1140 tggaacgtta cccagacact ctactgggca gttctgagag ggactttttc taccacccag 1200 aaactcagca gtatttcttt gaccgtgacc cagacatctt ccgccacatc ctgaatttct 1260 accgcactgg gaagctccac tatcctcgcc acgagtgcat ctctgcttac gatgaagaac 1320 tggccttctt tggcctcatc ccggaaatca tcggcgactg ctgttatgag gagtacaagg 1380 atcgcaggcg agagaacgcc gagcgcctgc aggacgacgc ggataccgac accgctgggg 1440 agagcgcctt gcccaccatg actgcaaggc agagggtctg gagggccttc gagaaccccc 1500 acaccagcac gatggccctg gtgttctact atgtcacggg gtttttcatt gccgtctctg 1560 tcatcgcgaa tgtggtggaa acagtgccgt gcggatcaag cccaggtcac attaaagaac 1620 tgccctgtgg agagcggtat gctgtggcct tcttctgctt ggacacggcc tgcgtcatga 1680 tcttcacagt tgagtatttg cttcgcctgg ctgcagcgcc tagtcgttac cgttttgtgc 1740 gtagtgtcat gagtatcatc gacgtggtgg ccatcctgcc ttattacatt gggctggtga 1800 tgacagacaa tgaggacgtc agcggagcct ttgtcacact ccgagtcttc cgggtcttca 1860 ggatctttaa gttttcccgc cactctcaag gcctgcgcat cctggggtac acactgaaga 1920 gttgtgcctc agaattgggc ttcttgcttt tctcgctcac catggctatc atcatcttcg 1980 ctacagttat gttctacgca gagaaggggt cttcggctag caagttcacc agcatccctg 2040 cagccttctg gtataccatc gtcaccatga caacactagg gtatggtgac atggtgccaa 2100 aaaccatagc agggaagatt tttggttcta tctgttcgct gagtggggtc ttggtcattg 2160 ctctacctgt tccggtgatt gtatccaact tcagtcgcat ctaccaccag aatcaacgag 2220 cagacaaacg aagggcacaa aagaaagcta gactggccag gatccgggca gccaaaagcg 2280 gaagcgcaaa tgcttacatg cagagcaaac ggaatggttt actcagtaat cagctgcagt 2340 cctcagagga tgagcaggct tttgttagca aatccggctc cagctttgaa acccagcacc 2400 accacctgct tcactgcctg gaaaaaacca cgaatcacga gtttgtggac gaacaagtct 2460 ttgaagaaag ctgcatggaa gttgcaactg ttaatcgtcc ttcaagtcac agtccttcac 2520 tgtcttcaca acaaggagtc accagcacct gctgttcacg acgacacaaa aaaacttttc 2580 gcatcccaaa tgccaatgta tcaggaagcc atcaaggtag tatacaagaa ctcagcacga 2640 ttcagatcag atgtgtggag agaacacctc tgtctaacag ccgatccagt ttaaatgcca 2700 aaatggaaga gtgtgttaaa ctaaactgtg aacaacctta tgtgactaca gcaataataa 2760 gcatcccaac acctccagta accacaccag aaggagacga taggccagaa tcccctgagt 2820 actcaggagg aaatattgtc agagtttctg ctttgtaaga caattggaat aaggtctaag 2880 agaattcgag ccctggctgt gaaaagaatc tcaacataga agaaagaaga aacaataaat 2940 attctgcaga ttaatgcagc aaagaaagaa ggttggtagt gaaacacaaa gcttccaatc 3000 ttaaggatgt gaataaaacc accaaatggc atttctagac agtttgacct gttatacaga 3060 gtaatattct gtggcccttt gactttgtga atgagcacaa tgaaatgccg cctactgatg 3120 cttcttatga tcagaactct tttttaataa aataaataac ataaatcgtt gaacataatg 3180 ttccagttga atgcaaaaca aaaaaaatat ggaaaacatt ttgataaaat tttttcctgt 3240 taaaaccatg aacattggct atgatgaaga ttattacata tgaaaaaaaa actcacacaa 3300 catatttgta ttgactgaag gaaaccatca taatgcatgc tagaattctt tgaagcagtg 3360 atctcagttt ccttatgttg tcttcagaat aggcatgata aactataatt gtagaaaggg 3420 gtaatttctg tgcacttaca acaagctgag tgttcatgtt ccatggtggg ctgtgcaaat 3480 aaactccttt tagacctgca gtatttctca tggggatgct cattagtaaa tctaaagtgt 3540 tcagatagtt cagtattcat tatcgtttaa ctttgcacct agatactgtt acaactgcaa 3600 taatttgttg tacaactgtt gtatcaggaa tcaggatttt tttgttgttg tactttccag 3660 atccttatag atacggtaag agccacattc gtagaaaaac ttctggtgtg gccaggtttt 3720 aggtaacttt ttaatccaaa actattgtgc cataaatgtt tttcagtaat attttttggt 3780 ccactgtatt cctgtgacac agtgcattat ctgttcttgt atttctatag cacctctcta 3840 ttgggtttat catcatcaac aagactactg tttactgtag ttcaagtgac tttcctactt 3900 ttgtatttcc aaaaaaaatt atcttgtaag tagcttgtca tcaatcccct tgtcgaaaac 3960 tagaaaaaaa ggagttgacc catataaatt atctctaacg tctttgttgt ttatggaaaa 4020 gcccagatac tggatatatc actatgtatt ttatgaacag aattgactgg gactaatatc 4080 acaggatcaa tcatctcaga atcttacttg atgcattatt tattttgctt tagatcttga 4140 atacattttg agaataacta atgtggattg aaatgtagag atacactgga gtgctttatt 4200 tagcaatatt tgatgaaagc atgctttcta cgccattcag gaaggcagca caaatttatc 4260 tcagaaaggt tcctgtgtat tgcaaggtac aattttctcc aataaatcag gagaacagga 4320 gtttgatgat gcaaagttga tctctgtaca tttaagtgaa aagtctttat aacttttcac 4380 ccttaaaata tttcagcaga catgtctgca catgacagtg taaaaaagtt taatgtcaaa 4440 tgcaaagttt ttattcattc caagccacca ctgtaaggaa taaagcttag cttctgtaca 4500 tggaaagagc taataattat ccctctgtca gagatgagat ttttaaatgc ttatgatatt 4560 taatcataaa aagggattaa tccaaccatt ttcaagtaaa gccagaaatt cttgcttccc 4620 atttctagaa tagtttctag aacagtgcta tgcacatatt agatcttaat aaacatttgc 4680 tgagtgaaag taagataaac tcaactatct cttgggaaga actggcttca ttcctagtac 4740 atcttttaaa aagttactaa ttttccagca gtacaaatat taacaattat attaacacct 4800 gcctcatgtc agtttatgct tctagagcaa tgtctagtga aacttatctg atggcattta 4860 ttgaaaacct tctaaaaagt agactaagga aaccataatc agaattacta tgtcttttga 4920 ttcccaatga gaagttctat tttcatgttc ttaatattac atacaagaaa atgcagttag 4980 gttatttcaa ttgacaattc tgcctcctct tttgatttat cacttaccca aaattattaa 5040 ttttattagg cttttggaaa agaaaaaaaa ctttttgatg ttttaggtga tttaaaaata 5100 taccgtgttg gtggtgaatg actattgatg actgtgttaa gtgcatctgt attgtaagtg 5160 aaatgtaatt atttctgtgt accatatgga gtaactaagg tcattgtttt tgacaatttt 5220 gtttgaaatt catatatctt atttcaaagg atagcataat atctgcatta tgctggaaaa 5280 aaatagacct ttggagaata cttaaataaa acatgtgcat gcttgaacag gac 5333 <210> SEQ ID NO 255 <211> LENGTH: 5404 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 255 ggagatgcag gaccacccac tggcggggaa gcagctagca gccctcccgc gcccccgcgc 60 tgccgagcgc cttctgcctc cgcgctcgga cgagagcccg tgccggcccc ggccccggcc 120 ccaccgcgcc aacgccgccc gcccggccgc cccgcagccc cgccgccccg cagccccgca 180 ccgcgctggc caggctcccg cgacagtggc cccgcagtaa gttggcagga gcgagtcccc 240 tccgttctcg cctcccccgc accttttgaa cttgttgctg ctgctctgct cgcctgcgcc 300 tggcttttgg aaggtgaaaa ggaggaggga ggcacggagg gatgggggaa gggaaagaag 360 agctcgcttg agctttattt atgctctctc ggcgcatcgg attcggctgc tcgcgagctg 420 ctttctctcc tcttcccttt ccgggtgcac ggcgaggaga aagtctctat gcaactaagc 480 cccggcgcgc acttggccag gtatgtaccg cgggagcggc gcgttctgcg cggaagcaga 540 tgctgctgcc gccacggcgg cggcggctgc cagctcctga gctctgtaac tgtcacactg 600 cacctgagct gaacttgaaa agagagtgaa ggggcgattg ggcgaacgct tttggcagac 660 acagagggtg tttgtagacg tgggggagga gaatctctat taacgccccc caccgtaacc 720 actgcacatc acctccatct ctgcaaatac agcccgagga gtagaggcag cagcagctgg 780 acccccaaag agagacgtgg ggcagcggct gtgaccgcat ctcctgagct acaacaacag 840 gtcgcctttt tgagactcct ttggcgggaa gggctacttg gaaaggaagg tttgaaagag 900 tgagaagggt aggtgtaagg gttccctaat tcgtcgaaag aattctattg ggtgactctc 960 gttcgtcttc tctatcctac actccacata ctgaccctat attatccaga ctgtgccggg 1020 gagaaatcaa aaacacctgt ttgaagaaac ggctgcacct gtgtgcttat ttgtgccaga 1080 gggtggccta gcccacctgc aggaagagat ttggctgggt tctgttgagg gtgattgtta 1140 ggacgttgta ttttgttgcc attattccaa atacctgtct tggagggaaa gttgcccttc 1200 tgagaactgt gactttacca ggagccctat cttggaataa gagttacacc tctggaccac 1260 gtttctcact agtactttgc ttgactggag gaagtgggtg acttttggct gcttcggtga 1320 cccattgtag acgcctcgtt acccttcttc cttccgcttc aagtaatcat ggcggcgggg 1380 gtggcagcgt ggctgccttt tgcaagggca gcggctatcg ggtggatgcc tgtggcctcg 1440 gggcctatgc cggctccccc gaggcaggag aggaaaagga cccaagatgc tctcattgtg 1500 ctgaatgtga gtggcacccg cttccagacg tggcaggaca ccctggaacg ttacccagac 1560 actctactgg gcagttctga gagggacttt ttctaccacc cagaaactca gcagtatttc 1620 tttgaccgtg acccagacat cttccgccac atcctgaatt tctaccgcac tgggaagctc 1680 cactatcctc gccacgagtg catctctgct tacgatgaag aactggcctt ctttggcctc 1740 atcccggaaa tcatcggcga ctgctgttat gaggagtaca aggatcgcag gcgagagaac 1800 gccgagcgcc tgcaggacga cgcggatacc gacaccgctg gggagagcgc cttgcccacc 1860 atgactgcaa ggcagagggt ctggagggcc ttcgagaacc cccacaccag cacgatggcc 1920 ctggtgttct actatgtcac ggggtttttc attgccgtct ctgtcatcgc gaatgtggtg 1980 gaaacagtgc cgtgcggatc aagcccaggt cacattaaag aactgccctg tggagagcgg 2040 tatgctgtgg ccttcttctg cttggacacg gcctgcgtca tgatcttcac agttgagtat 2100 ttgcttcgcc tggctgcagc gcctagtcgt taccgttttg tgcgtagtgt catgagtatc 2160 atcgacgtgg tggccatcct gccttattac attgggctgg tgatgacaga caatgaggac 2220 gtcagcggag cctttgtcac actccgagtc ttccgggtct tcaggatctt taagttttcc 2280 cgccactctc aaggcctgcg catcctgggg tacacactga agagttgtgc ctcagaattg 2340 ggcttcttgc ttttctcgct caccatggct atcatcatct tcgctacagt tatgttctac 2400 gcagagaagg ggtcttcggc tagcaagttc accagcatcc ctgcagcctt ctggtatacc 2460 atcgtcacca tgacaacact agggtaggtg ccataatggg aaatgggatg gaggttgggt 2520 atgggtgagg cgattgtgga cccatcgagg ttacatggta actccgggga aatcatttgt 2580 tttctttcct gagtttagga aagcattatc taaatggttt ggcaaaactc ttttcatctg 2640 tgaaatgggt ataatacaca cgttgaagta ttaaggcatt gctggcaaat gttgatgcct 2700 gaaagtgata aagatacaaa gaaattttag aattcctgaa tatatgaaag tagtagcaat 2760 atttatatta atatataaaa atatgacaat gaaaaacaaa atctatgccc taataaagac 2820 acaaatatat acaatgtata ttgaaatgtc tataaagtgg ttcaatgcat ttaaatgaaa 2880 agtttccagg tatacttgaa ctattatttt catatgaata gatacttatg gtgtacattt 2940 ttcctctaag aaccataatt cctattttac atcgtaatac atagattgta gatgtaatta 3000 tcaaagtatt ttataatata tatgcacata ttcatatgta tgcactttaa ttatggttga 3060 taggttattc agtcttttag aatatcagag ctgaaactga tcaactctac aatatgcagt 3120 ggaattaaat ttgcaacata tttcaagctc taggttcata gtttcaaaaa aagaagcaaa 3180 agactgtcat ccacacattt ttttttagaa tctacagatc ccatcaggca atgggtccac 3240 acccattaaa tacacataga agatagagca gtatctggta agattgatgg tcaccaaggc 3300 tggctgtatt ataaaatttg gggtcctaat ttccttttag aatttttttg tgaattcttt 3360 tttgggggta taatgaagtt ctgcaaccaa agggacaaat ttctgaattc atgctgttgt 3420 ttttaatata cttttagggc tagaattaag tttttttagg tagtagagaa aaggaaagga 3480 ggcaaatgat taataatgtt aaactgcaga aaagtagcag cattttacat attagagaat 3540 ctaataaaat aaaatggtta gatcttttta cttttatgag ttcttagata agctggggag 3600 tgatgtgagt gccttttctt cagctttgtg ctactattct tgcataggta atcagtttag 3660 tgaggatttg gtaatggcta taagaaaaaa gttattccca aggctactct ttaagctttg 3720 tgtttttgga taatttaatt ggcttcttta aatgacattg tggttaaagt caacttaatt 3780 ttattagaca tattgtgttg tacagaattt ctcatgtcat gtggccagct aatggaatag 3840 tttatatatg aagaatttta ggctaggtta aacaagaaat tggggtaaag aaaaatacaa 3900 tgatttatga tttttattta gtctcatttt tttaaagacc tactggtaca tttaaaaaat 3960 gaattagtga aaatccatgt tctacttctt atatttcctt tttatcttgt tggcaaattt 4020 gtgacagttt ataaggataa ggatgatgca gaatgccttc gcagtgtagg tgctgattct 4080 ttatcaaaga ggtttgtttt tgttgtcttg tcattttgta gcaggagatc cttattaagg 4140 acaaatgggt agtgcaaatc accatcatga cgtcaaatta gaagtacact tgaataaaaa 4200 agattctgtt ttaataggaa gggagaacta ttaaaatgaa atacacttta aaaatttggt 4260 atatatggct gtgtttcttg aggtatcagt gaatcatttt aatgctatat agtgtctata 4320 tgattgaata taggtataaa aagaatgttg atgagaattc taatttcata tagctaatag 4380 ttctatacta gacttgagaa gttagcatta ttttaaaact tgtttctgga aatgactttc 4440 caatttttat tttattttga agcttatttt tgtttcaagg aaaatatgag acaacattaa 4500 acattagtga caatttttta ttatgtaaat aaaatactta aaagcaccca tttttgaaaa 4560 tatttaagaa attgaattat attgcctgag taaaatctat gcagtggatt tagttcacat 4620 gtttcatagg taagtaagtg gattagaagc attgaataca cacgctttct cagaacttgg 4680 aagctaagtg gaagttactt taaagactta gcttcactga atttgaacat tttaattttc 4740 aggaaattaa gctaattaat gatcctgatg gaatagagca gtcatacttt taagatgtgg 4800 aaatgtcgat gtaatcaaaa tgagaacata tatggacact tgacaaatca tatgctttat 4860 aatataacag aatttcatag aaaaatgtct ttaatttctc atcaaaatgt attatgtatt 4920 gtaccctgaa gaaacagatt cttataagcc ctgccttttt ggtgccatct ttgtgactca 4980 gttatttaat aatacaaaat attcaataaa agccattgcc taactttatt gtttaggctg 5040 tagttctata cttagaggat gaagtgtaag gtgcaaactt tctgggaaat aatagttgaa 5100 gccaatatcc aactatgtct gaatgattat caagagttat ctgagctctt tttatggggc 5160 tattaatttt aatggagcta aatgttcttc aattagtgat aatagaagtg aaaatgtgat 5220 tgtaaacagt ggttattgaa agttccatct cgtatgaacg ttatctacat gagaataaat 5280 aaccaagagc tttgtcattc aggactggca gaatcatttg cagcttctag agtattttag 5340 acaatattca gttggtttta tgatctaaag aactgagtgt gtctatctta gaaccaaggt 5400 gtat 5404 <210> SEQ ID NO 256 <211> LENGTH: 1597 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 256 cggctgctcg cgagctgctt tctctcctct tccctttccg ggtgcacggc gaggagaaag 60 tctctatgca actaagcccc ggcgcgcact tggccaggta tgtaccgcgg gagcggcgcg 120 ttctgcgcgg aagcagatgc tgctgccgcc acggcggcgg cggctgccag ctcctgagct 180 ctgtaactgt cacactgcac ctgagctgaa cttgaaaaga gagtgaaggg gcgattgggc 240 gaacgctttt ggcagacaca gagggtgttt gtagacgtgg gggaggagaa tctctattaa 300 cgccccccac cgtaaccact gcacatcacc tccatctctg caaatacagc ccgaggagta 360 gaggcagcag cagctggacc cccaaagaga gacgtggggc agcggctgtg accgcatctc 420 ctgagctaca acaacaggtc gcctttttga gactcctttg gcgggaaggg ctacttggaa 480 aggaaggttt gaaagagtga gaagggtagg tgtaagggtt ccctaattcg tcgaaagaat 540 tctattgggt gactctcgtt cgtcttctct atcctacact ccacatactg accctatatt 600 atccagactg tgccggggag aaatcaaaaa cacctgtttg aagaaacggc tgcacctgtg 660 tgcttatttg tgccagaggg tggcctagcc cacctgcagg aagagatttg gctgggttct 720 gttgagggtg attgttagga cgttgtattt tgttgccatt attccaaata cctgtcttgg 780 agggaaagtt gcccttctga gaactgtgac tttaccagga gccctatctt ggaataagag 840 ttacacctct ggaccacgtt tctcactagt actttgcttg actggaggaa gtgggtgact 900 tttggctgct tcggtgaccc attgtagacg cctcgttacc cttcttcctt ccgcttcaag 960 taatcatggc ggcgggggtg gcagcgtggc tgccttttgc aagggcagcg gctatcgggt 1020 ggatgcctgt ggcctcgggg cctatgccgg ctcccccgag gcaggagagg aaaaggaccc 1080 aagatgctct cattgtgctg aatgtgagtg gcacccgctt ccagacgtgg caggacaccc 1140 tggaacgtta cccagacact ctactgggca gttctgagag ggactttttc taccacccag 1200 aaactcagca gtatttcttt gaccgtgacc cagacatctt ccgccacatc ctgaatttct 1260 accgcactgg gaagctccac tatcctcgcc acgagtgcat ctctgcttac gatgaagaac 1320 tggccttctt tggcctcatc ccggaaatca tcggcgactg ctgttatgag gagtacaagg 1380 atcgcaggcg agagaacgcc gagcgcctgc aggacgacgc ggataccgac accgctgggg 1440 agagcgcctt gcccaccatg actgcaaggc agagggtctg gagggccttc gagaaccccc 1500 acaccagcac gatggccctg gtgttctact atgtcacggg gtttttcatt gccgtctctg 1560 tcatcgcgaa tgtggtggaa acagtgccgt gcggatc 1597 <210> SEQ ID NO 257 <211> LENGTH: 255 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 257 Met Val Pro Lys Thr Ile Ala Gly Lys Ile Phe Gly Ser Ile Cys Ser 5 10 15 Leu Ser Gly Val Leu Val Ile Ala Leu Pro Val Pro Val Ile Val Ser 20 25 30 Asn Phe Ser Arg Ile Tyr His Gln Asn Gln Arg Ala Asp Lys Arg Arg 35 40 45 Ala Gln Lys Lys Ala Arg Leu Ala Arg Ile Arg Ala Ala Lys Ser Gly 50 55 60 Ser Ala Asn Ala Tyr Met Gln Ser Lys Arg Asn Gly Leu Leu Ser Asn 65 70 75 80 Gln Leu Gln Ser Ser Glu Asp Glu Gln Ala Phe Val Ser Lys Ser Gly 85 90 95 Ser Ser Phe Glu Thr Gln His His His Leu Leu His Cys Leu Glu Lys 100 105 110 Thr Thr Asn His Glu Phe Val Asp Glu Gln Val Phe Glu Glu Ser Cys 115 120 125 Met Glu Val Ala Thr Val Asn Arg Pro Ser Ser His Ser Pro Ser Leu 130 135 140 Ser Ser Gln Gln Gly Val Thr Ser Thr Cys Cys Ser Arg Arg His Lys 145 150 155 160 Lys Thr Phe Arg Ile Pro Asn Ala Asn Val Ser Gly Ser His Gln Gly 165 170 175 Ser Ile Gln Glu Leu Ser Thr Ile Gln Ile Arg Cys Val Glu Arg Thr 180 185 190 Pro Leu Ser Asn Ser Arg Ser Ser Leu Asn Ala Lys Met Glu Glu Cys 195 200 205 Val Lys Leu Asn Cys Glu Gln Pro Tyr Val Thr Thr Ala Ile Ile Ser 210 215 220 Ile Pro Thr Pro Pro Val Thr Thr Pro Glu Gly Asp Asp Arg Pro Glu 225 230 235 240 Ser Pro Glu Tyr Ser Gly Gly Asn Ile Val Arg Val Ser Ala Leu 245 250 255 <210> SEQ ID NO 258 <211> LENGTH: 630 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 258 Met Ala Ala Gly Val Ala Ala Trp Leu Pro Phe Ala Arg Ala Ala Ala 5 10 15 Ile Gly Trp Met Pro Val Ala Ser Gly Pro Met Pro Ala Pro Pro Arg 20 25 30 Gln Glu Arg Lys Arg Thr Gln Asp Ala Leu Ile Val Leu Asn Val Ser 35 40 45 Gly Thr Arg Phe Gln Thr Trp Gln Asp Thr Leu Glu Arg Tyr Pro Asp 50 55 60 Thr Leu Leu Gly Ser Ser Glu Arg Asp Phe Phe Tyr His Pro Glu Thr 65 70 75 80 Gln Gln Tyr Phe Phe Asp Arg Asp Pro Asp Ile Phe Arg His Ile Leu 85 90 95 Asn Phe Tyr Arg Thr Gly Lys Leu His Tyr Pro Arg His Glu Cys Ile 100 105 110 Ser Ala Tyr Asp Glu Glu Leu Ala Phe Phe Gly Leu Ile Pro Glu Ile 115 120 125 Ile Gly Asp Cys Cys Tyr Glu Glu Tyr Lys Asp Arg Arg Arg Glu Asn 130 135 140 Ala Glu Arg Leu Gln Asp Asp Ala Asp Thr Asp Thr Ala Gly Glu Ser 145 150 155 160 Ala Leu Pro Thr Met Thr Ala Arg Gln Arg Val Trp Arg Ala Phe Glu 165 170 175 Asn Pro His Thr Ser Thr Met Ala Leu Val Phe Tyr Tyr Val Thr Gly 180 185 190 Phe Phe Ile Ala Val Ser Val Ile Ala Asn Val Val Glu Thr Val Pro 195 200 205 Cys Gly Ser Ser Pro Gly His Ile Lys Glu Leu Pro Cys Gly Glu Arg 210 215 220 Tyr Ala Val Ala Phe Phe Cys Leu Asp Thr Ala Cys Val Met Ile Phe 225 230 235 240 Thr Val Glu Tyr Leu Leu Arg Leu Ala Ala Ala Pro Ser Arg Tyr Arg 245 250 255 Phe Val Arg Ser Val Met Ser Ile Ile Asp Val Val Ala Ile Leu Pro 260 265 270 Tyr Tyr Ile Gly Leu Val Met Thr Asp Asn Glu Asp Val Ser Gly Ala 275 280 285 Phe Val Thr Leu Arg Val Phe Arg Val Phe Arg Ile Phe Lys Phe Ser 290 295 300 Arg His Ser Gln Gly Leu Arg Ile Leu Gly Tyr Thr Leu Lys Ser Cys 305 310 315 320 Ala Ser Glu Leu Gly Phe Leu Leu Phe Ser Leu Thr Met Ala Ile Ile 325 330 335 Ile Phe Ala Thr Val Met Phe Tyr Ala Glu Lys Gly Ser Ser Ala Ser 340 345 350 Lys Phe Thr Ser Ile Pro Ala Ala Phe Trp Tyr Thr Ile Val Thr Met 355 360 365 Thr Thr Leu Gly Tyr Gly Asp Met Val Pro Lys Thr Ile Ala Gly Lys 370 375 380 Ile Phe Gly Ser Ile Cys Ser Leu Ser Gly Val Leu Val Ile Ala Leu 385 390 395 400 Pro Val Pro Val Ile Val Ser Asn Phe Ser Arg Ile Tyr His Gln Asn 405 410 415 Gln Arg Ala Asp Lys Arg Arg Ala Gln Lys Lys Ala Arg Leu Ala Arg 420 425 430 Ile Arg Ala Ala Lys Ser Gly Ser Ala Asn Ala Tyr Met Gln Ser Lys 435 440 445 Arg Asn Gly Leu Leu Ser Asn Gln Leu Gln Ser Ser Glu Asp Glu Gln 450 455 460 Ala Phe Val Ser Lys Ser Gly Ser Ser Phe Glu Thr Gln His His His 465 470 475 480 Leu Leu His Cys Leu Glu Lys Thr Thr Asn His Glu Phe Val Asp Glu 485 490 495 Gln Val Phe Glu Glu Ser Cys Met Glu Val Ala Thr Val Asn Arg Pro 500 505 510 Ser Ser His Ser Pro Ser Leu Ser Ser Gln Gln Gly Val Thr Ser Thr 515 520 525 Cys Cys Ser Arg Arg His Lys Lys Thr Phe Arg Ile Pro Asn Ala Asn 530 535 540 Val Ser Gly Ser His Gln Gly Ser Ile Gln Glu Leu Ser Thr Ile Gln 545 550 555 560 Ile Arg Cys Val Glu Arg Thr Pro Leu Ser Asn Ser Arg Ser Ser Leu 565 570 575 Asn Ala Lys Met Glu Glu Cys Val Lys Leu Asn Cys Glu Gln Pro Tyr 580 585 590 Val Thr Thr Ala Ile Ile Ser Ile Pro Thr Pro Pro Val Thr Thr Pro 595 600 605 Glu Gly Asp Asp Arg Pro Glu Ser Pro Glu Tyr Ser Gly Gly Asn Ile 610 615 620 Val Arg Val Ser Ala Leu 625 630 <210> SEQ ID NO 259 <211> LENGTH: 630 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 259 Met Ala Ala Gly Val Ala Ala Trp Leu Pro Phe Ala Arg Ala Ala Ala 5 10 15 Ile Gly Trp Met Pro Val Ala Ser Gly Pro Met Pro Ala Pro Pro Arg 20 25 30 Gln Glu Arg Lys Arg Thr Gln Asp Ala Leu Ile Val Leu Asn Val Ser 35 40 45 Gly Thr Arg Phe Gln Thr Trp Gln Asp Thr Leu Glu Arg Tyr Pro Asp 50 55 60 Thr Leu Leu Gly Ser Ser Glu Arg Asp Phe Phe Tyr His Pro Glu Thr 65 70 75 80 Gln Gln Tyr Phe Phe Asp Arg Asp Pro Asp Ile Phe Arg His Ile Leu 85 90 95 Asn Phe Tyr Arg Thr Gly Lys Leu His Tyr Pro Arg His Glu Cys Ile 100 105 110 Ser Ala Tyr Asp Glu Glu Leu Ala Phe Phe Gly Leu Ile Pro Glu Ile 115 120 125 Ile Gly Asp Cys Cys Tyr Glu Glu Tyr Lys Asp Arg Arg Arg Glu Asn 130 135 140 Ala Glu Arg Leu Gln Asp Asp Ala Asp Thr Asp Thr Ala Gly Glu Ser 145 150 155 160 Ala Leu Pro Thr Met Thr Ala Arg Gln Arg Val Trp Arg Ala Phe Glu 165 170 175 Asn Pro His Thr Ser Thr Met Ala Leu Val Phe Tyr Tyr Val Thr Gly 180 185 190 Phe Phe Ile Ala Val Ser Val Ile Ala Asn Val Val Glu Thr Val Pro 195 200 205 Cys Gly Ser Ser Pro Gly His Ile Lys Glu Leu Pro Cys Gly Glu Arg 210 215 220 Tyr Ala Val Ala Phe Phe Cys Leu Asp Thr Ala Cys Val Met Ile Phe 225 230 235 240 Thr Val Glu Tyr Leu Leu Arg Leu Ala Ala Ala Pro Ser Arg Tyr Arg 245 250 255 Phe Val Arg Ser Val Met Ser Ile Ile Asp Val Val Ala Ile Leu Pro 260 265 270 Tyr Tyr Ile Gly Leu Val Met Thr Asp Asn Glu Asp Val Ser Gly Ala 275 280 285 Phe Val Thr Leu Arg Val Phe Arg Val Phe Arg Ile Phe Lys Phe Ser 290 295 300 Arg His Ser Gln Gly Leu Arg Ile Leu Gly Tyr Thr Leu Lys Ser Cys 305 310 315 320 Ala Ser Glu Leu Gly Phe Leu Leu Phe Ser Leu Thr Met Ala Ile Ile 325 330 335 Ile Phe Ala Thr Val Met Phe Tyr Ala Glu Lys Gly Ser Ser Ala Ser 340 345 350 Lys Phe Thr Ser Ile Pro Ala Ala Phe Trp Tyr Thr Ile Val Thr Met 355 360 365 Thr Thr Leu Gly Tyr Gly Asp Met Val Pro Lys Thr Ile Ala Gly Lys 370 375 380 Ile Phe Gly Ser Ile Cys Ser Leu Ser Gly Val Leu Val Ile Ala Leu 385 390 395 400 Pro Val Pro Val Ile Val Ser Asn Phe Ser Arg Ile Tyr His Gln Asn 405 410 415 Gln Arg Ala Asp Lys Arg Arg Ala Gln Lys Lys Ala Arg Leu Ala Arg 420 425 430 Ile Arg Ala Ala Lys Ser Gly Ser Ala Asn Ala Tyr Met Gln Ser Lys 435 440 445 Arg Asn Gly Leu Leu Ser Asn Gln Leu Gln Ser Ser Glu Asp Glu Gln 450 455 460 Ala Phe Val Ser Lys Ser Gly Ser Ser Phe Glu Thr Gln His His His 465 470 475 480 Leu Leu His Cys Leu Glu Lys Thr Thr Asn His Glu Phe Val Asp Glu 485 490 495 Gln Val Phe Glu Glu Ser Cys Met Glu Val Ala Thr Val Asn Arg Pro 500 505 510 Ser Ser His Ser Pro Ser Leu Ser Ser Gln Gln Gly Val Thr Ser Thr 515 520 525 Cys Cys Ser Arg Arg His Lys Lys Thr Phe Arg Ile Pro Asn Ala Asn 530 535 540 Val Ser Gly Ser His Gln Gly Ser Ile Gln Glu Leu Ser Thr Ile Gln 545 550 555 560 Ile Arg Cys Val Glu Arg Thr Pro Leu Ser Asn Ser Arg Ser Ser Leu 565 570 575 Asn Ala Lys Met Glu Glu Cys Val Lys Leu Asn Cys Glu Gln Pro Tyr 580 585 590 Val Thr Thr Ala Ile Ile Ser Ile Pro Thr Pro Pro Val Thr Thr Pro 595 600 605 Glu Gly Asp Asp Arg Pro Glu Ser Pro Glu Tyr Ser Gly Gly Asn Ile 610 615 620 Val Arg Val Ser Ala Leu 625 630 <210> SEQ ID NO 260 <211> LENGTH: 630 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 260 Met Ala Ala Gly Val Ala Ala Trp Leu Pro Phe Ala Arg Ala Ala Ala 5 10 15 Ile Gly Trp Met Pro Val Ala Ser Gly Pro Met Pro Ala Pro Pro Arg 20 25 30 Gln Glu Arg Lys Arg Thr Gln Asp Ala Leu Ile Val Leu Asn Val Ser 35 40 45 Gly Thr Arg Phe Gln Thr Trp Gln Asp Thr Leu Glu Arg Tyr Pro Asp 50 55 60 Thr Leu Leu Gly Ser Ser Glu Arg Asp Phe Phe Tyr His Pro Glu Thr 65 70 75 80 Gln Gln Tyr Phe Phe Asp Arg Asp Pro Asp Ile Phe Arg His Ile Leu 85 90 95 Asn Phe Tyr Arg Thr Gly Lys Leu His Tyr Pro Arg His Glu Cys Ile 100 105 110 Ser Ala Tyr Asp Glu Glu Leu Ala Phe Phe Gly Leu Ile Pro Glu Ile 115 120 125 Ile Gly Asp Cys Cys Tyr Glu Glu Tyr Lys Asp Arg Arg Arg Glu Asn 130 135 140 Ala Glu Arg Leu Gln Asp Asp Ala Asp Thr Asp Thr Ala Gly Glu Ser 145 150 155 160 Ala Leu Pro Thr Met Thr Ala Arg Gln Arg Val Trp Arg Ala Phe Glu 165 170 175 Asn Pro His Thr Ser Thr Met Ala Leu Val Phe Tyr Tyr Val Thr Gly 180 185 190 Phe Phe Ile Ala Val Ser Val Ile Ala Asn Val Val Glu Thr Val Pro 195 200 205 Cys Gly Ser Ser Pro Gly His Ile Lys Glu Leu Pro Cys Gly Glu Arg 210 215 220 Tyr Ala Val Ala Phe Phe Cys Leu Asp Thr Ala Cys Val Met Ile Phe 225 230 235 240 Thr Val Glu Tyr Leu Leu Arg Leu Ala Ala Ala Pro Ser Arg Tyr Arg 245 250 255 Phe Val Arg Ser Val Met Ser Ile Ile Asp Val Val Ala Ile Leu Pro 260 265 270 Tyr Tyr Ile Gly Leu Val Met Thr Asp Asn Glu Asp Val Ser Gly Ala 275 280 285 Phe Val Thr Leu Arg Val Phe Arg Val Phe Arg Ile Phe Lys Phe Ser 290 295 300 Arg His Ser Gln Gly Leu Arg Ile Leu Gly Tyr Thr Leu Lys Ser Cys 305 310 315 320 Ala Ser Glu Leu Gly Phe Leu Leu Phe Ser Leu Thr Met Ala Ile Ile 325 330 335 Ile Phe Ala Thr Val Met Phe Tyr Ala Glu Lys Gly Ser Ser Ala Ser 340 345 350 Lys Phe Thr Ser Ile Pro Ala Ala Phe Trp Tyr Thr Ile Val Thr Met 355 360 365 Thr Thr Leu Gly Tyr Gly Asp Met Val Pro Lys Thr Ile Ala Gly Lys 370 375 380 Ile Phe Gly Ser Ile Cys Ser Leu Ser Gly Val Leu Val Ile Ala Leu 385 390 395 400 Pro Val Pro Val Ile Val Ser Asn Phe Ser Arg Ile Tyr His Gln Asn 405 410 415 Gln Arg Ala Asp Lys Arg Arg Ala Gln Lys Lys Ala Arg Leu Ala Arg 420 425 430 Ile Arg Ala Ala Lys Ser Gly Ser Ala Asn Ala Tyr Met Gln Ser Lys 435 440 445 Arg Asn Gly Leu Leu Ser Asn Gln Leu Gln Ser Ser Glu Asp Glu Gln 450 455 460 Ala Phe Val Ser Lys Ser Gly Ser Ser Phe Glu Thr Gln His His His 465 470 475 480 Leu Leu His Cys Leu Glu Lys Thr Thr Asn His Glu Phe Val Asp Glu 485 490 495 Gln Val Phe Glu Glu Ser Cys Met Glu Val Ala Thr Val Asn Arg Pro 500 505 510 Ser Ser His Ser Pro Ser Leu Ser Ser Gln Gln Gly Val Thr Ser Thr 515 520 525 Cys Cys Ser Arg Arg His Lys Lys Thr Phe Arg Ile Pro Asn Ala Asn 530 535 540 Val Ser Gly Ser His Gln Gly Ser Ile Gln Glu Leu Ser Thr Ile Gln 545 550 555 560 Ile Arg Cys Val Glu Arg Thr Pro Leu Ser Asn Ser Arg Ser Ser Leu 565 570 575 Asn Ala Lys Met Glu Glu Cys Val Lys Leu Asn Cys Glu Gln Pro Tyr 580 585 590 Val Thr Thr Ala Ile Ile Ser Ile Pro Thr Pro Pro Val Thr Thr Pro 595 600 605 Glu Gly Asp Asp Arg Pro Glu Ser Pro Glu Tyr Ser Gly Gly Asn Ile 610 615 620 Val Arg Val Ser Ala Leu 625 630 <210> SEQ ID NO 261 <211> LENGTH: 630 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 261 Met Ala Ala Gly Val Ala Ala Trp Leu Pro Phe Ala Arg Ala Ala Ala 5 10 15 Ile Gly Trp Met Pro Val Ala Ser Gly Pro Met Pro Ala Pro Pro Arg 20 25 30 Gln Glu Arg Lys Arg Thr Gln Asp Ala Leu Ile Val Leu Asn Val Ser 35 40 45 Gly Thr Arg Phe Gln Thr Trp Gln Asp Thr Leu Glu Arg Tyr Pro Asp 50 55 60 Thr Leu Leu Gly Ser Ser Glu Arg Asp Phe Phe Tyr His Pro Glu Thr 65 70 75 80 Gln Gln Tyr Phe Phe Asp Arg Asp Pro Asp Ile Phe Arg His Ile Leu 85 90 95 Asn Phe Tyr Arg Thr Gly Lys Leu His Tyr Pro Arg His Glu Cys Ile 100 105 110 Ser Ala Tyr Asp Glu Glu Leu Ala Phe Phe Gly Leu Ile Pro Glu Ile 115 120 125 Ile Gly Asp Cys Cys Tyr Glu Glu Tyr Lys Asp Arg Arg Arg Glu Asn 130 135 140 Ala Glu Arg Leu Gln Asp Asp Ala Asp Thr Asp Thr Ala Gly Glu Ser 145 150 155 160 Ala Leu Pro Thr Met Thr Ala Arg Gln Arg Val Trp Arg Ala Phe Glu 165 170 175 Asn Pro His Thr Ser Thr Met Ala Leu Val Phe Tyr Tyr Val Thr Gly 180 185 190 Phe Phe Ile Ala Val Ser Val Ile Ala Asn Val Val Glu Thr Val Pro 195 200 205 Cys Gly Ser Ser Pro Gly His Ile Lys Glu Leu Pro Cys Gly Glu Arg 210 215 220 Tyr Ala Val Ala Phe Phe Cys Leu Asp Thr Ala Cys Val Met Ile Phe 225 230 235 240 Thr Val Glu Tyr Leu Leu Arg Leu Ala Ala Ala Pro Ser Arg Tyr Arg 245 250 255 Phe Val Arg Ser Val Met Ser Ile Ile Asp Val Val Ala Ile Leu Pro 260 265 270 Tyr Tyr Ile Gly Leu Val Met Thr Asp Asn Glu Asp Val Ser Gly Ala 275 280 285 Phe Val Thr Leu Arg Val Phe Arg Val Phe Arg Ile Phe Lys Phe Ser 290 295 300 Arg His Ser Gln Gly Leu Arg Ile Leu Gly Tyr Thr Leu Lys Ser Cys 305 310 315 320 Ala Ser Glu Leu Gly Phe Leu Leu Phe Ser Leu Thr Met Ala Ile Ile 325 330 335 Ile Phe Ala Thr Val Met Phe Tyr Ala Glu Lys Gly Ser Ser Ala Ser 340 345 350 Lys Phe Thr Ser Ile Pro Ala Ala Phe Trp Tyr Thr Ile Val Thr Met 355 360 365 Thr Thr Leu Gly Tyr Gly Asp Met Val Pro Lys Thr Ile Ala Gly Lys 370 375 380 Ile Phe Gly Ser Ile Cys Ser Leu Ser Gly Val Leu Val Ile Ala Leu 385 390 395 400 Pro Val Pro Val Ile Val Ser Asn Phe Ser Arg Ile Tyr His Gln Asn 405 410 415 Gln Arg Ala Asp Lys Arg Arg Ala Gln Lys Lys Ala Arg Leu Ala Arg 420 425 430 Ile Arg Ala Ala Lys Ser Gly Ser Ala Asn Ala Tyr Met Gln Ser Lys 435 440 445 Arg Asn Gly Leu Leu Ser Asn Gln Leu Gln Ser Ser Glu Asp Glu Gln 450 455 460 Ala Phe Val Ser Lys Ser Gly Ser Ser Phe Glu Thr Gln His His His 465 470 475 480 Leu Leu His Cys Leu Glu Lys Thr Thr Asn His Glu Phe Val Asp Glu 485 490 495 Gln Val Phe Glu Glu Ser Cys Met Glu Val Ala Thr Val Asn Arg Pro 500 505 510 Ser Ser His Ser Pro Ser Leu Ser Ser Gln Gln Gly Val Thr Ser Thr 515 520 525 Cys Cys Ser Arg Arg His Lys Lys Thr Phe Arg Ile Pro Asn Ala Asn 530 535 540 Val Ser Gly Ser His Gln Gly Ser Ile Gln Glu Leu Ser Thr Ile Gln 545 550 555 560 Ile Arg Cys Val Glu Arg Thr Pro Leu Ser Asn Ser Arg Ser Ser Leu 565 570 575 Asn Ala Lys Met Glu Glu Cys Val Lys Leu Asn Cys Glu Gln Pro Tyr 580 585 590 Val Thr Thr Ala Ile Ile Ser Ile Pro Thr Pro Pro Val Thr Thr Pro 595 600 605 Glu Gly Asp Asp Arg Pro Glu Ser Pro Glu Tyr Ser Gly Gly Asn Ile 610 615 620 Val Arg Val Ser Ala Leu 625 630 <210> SEQ ID NO 262 <211> LENGTH: 2707 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 262 ggcaggccga gccagccgtg cgccgcgctc cagggcccag ggcgccgcac acgcacccac 60 ccacccaccc agcctcgcag cgccatgggc aagaacaagc agccacgcgg ccagcagagg 120 caggggggcc cgccggccgc ggacgccgct gggcccgacg acatggagcc gaagaagggc 180 acgggggccc ccaaggagtg cggggaggag gagccccgga cctgctgcgg ctgccggttc 240 ccgctgctgc tcgccctgct gcagctggcc ctgggcatcg ccgtgaccgt ggtgggcttc 300 ctcatggcga gcatcagctc ctccctgcta gtcagggaca ctccattttg ggctgggatc 360 attgtctgct tagtggccta tcttggcttg tttatgcttt gtgtctcata tcaggttgac 420 gaacggacat gtattcaatt ttctatgaaa ctgttatact ttctgctgag tgccctgggc 480 ctgacggtct gtgtgctggc cgtggccttt gccgcccacc actattcgca gctcacacag 540 tttacctgtg agaccacact cgactcttgc cagtgcaaac tgccctcctc ggagccgctc 600 agcaggacct ttgtttaccg ggatgtgacg gactgtacca gcgtcactgg cactttcaaa 660 ctgttcttac tcatccagat gattcttaat ttggtctgcg gccttgtgtg cttgttggcc 720 tgctttgtga tgtggaaaca taggtaccag gtcttctatg tgggtgtcag gatatgctcc 780 ctcacggctt ccgaaggccc ccagcaaaag atctaacatt cttgctcaaa gttgcgagag 840 aaagtagcac atggagtagc tgaggttaaa caaacaaaaa aaaattttaa acaaagaaag 900 gaaaaaaatt gacaataaaa gtcactcttc taattgaata tttttatatt tttatgaaac 960 aaaagagcat ttcttcaggt ttctattgta ttttttttaa cattcttgca gagaaagcaa 1020 gatccaaatt gattttggga tattaaaagt taacagaaca ctgaacaagg aaagaatggc 1080 atagatctat ctttacagtc tggagttaat tcctgttaac tcattttatc cattccttac 1140 ataatcttct ttcctgttag tccagtttga tggtgtgaat ggtgaatttc aggcccagtt 1200 gctaaatttt gtggcatctt cctctagtcc ttcccacctc cagtcatcag ccccactctg 1260 tcttggagac aggcaggagg tgggggaaga gctgaatctc tttattttcc ctggtagaga 1320 catcttcaag gcatgaaata gcttaaagag cagagtagaa atggaagagg ctttgcaaaa 1380 ggctagataa ctaacaacac ctgggttggg gcggcggcct cttctcttca gctcccttag 1440 cttggctccg taagtggatc acttgccaaa tgctttagat gattgcctct caataattga 1500 aaggtggtgg tagttgtatt ctaaatgatg tagaaggttt aaaaataatt acattatgct 1560 tctattctat catctaaaac aaatcattaa aactaatttc tagctaattg ttaattataa 1620 ttatgctcag aagtctattt aatgagctct gactgtactt acgctgcact gtcggtgtta 1680 agagaaatta ctctcacaag agcagaggcc tgaagattct ttcttctgaa agccaagcac 1740 cacaaggaaa aaaaaattat taatagctca ggttaaaaac acccatttaa acaaaaacaa 1800 gagcatttgt aataggaagt gtttatacaa acagcacatt tgtgatatgt tgaaaagcat 1860 ctctcttggc aaccaatcta tgtttgagga agattgggta atgctgatgt gttccattca 1920 tgaaactgta tttgatacat aatcctatta ttaattcgta tgcttagtca acctaggaaa 1980 tcaaaataat gttttgaagt tcttatttga gcaatatggc cttgacttgg agggtagttt 2040 tagttgtttt gtttttaagt gactgtggtt taaagcacaa atgccccaag gtggggagac 2100 ttctctctgt gattattgtt gctattaaat tctgaactgt atccatattt taaggaagga 2160 gctaaaaatg gaaattcatg aaacataaat ggtatcaaga actttatcag tatgctttgt 2220 tgaaagcaga aattaagata ataattgagt tcaattcgcc tctccgcatt gcctattgat 2280 acactttact aatcatgaaa ttctaaccta aaaggaaaac attttcctgc ttgtcttaga 2340 agaaagtgga ataattccac tgattgtgat aatggtttca atttctacac aatataaata 2400 tccagtataa aggaaagcgt taagtcggta agctagagga ttgtaaatat cttttatgtc 2460 ctctagataa aacacccgat taacagatgt taaacctttt aatgttttga tttgctttaa 2520 aaatggcctt cctacacatt agctccagct aaaaagacac attggagagc ttagaggata 2580 agtctctgga gcagaattta tcacacacaa aagttacacc aacagaatac caagcagaat 2640 gatgaggacc tgtaaaatac cttgtgccct attaaaaaaa aaaaaaaaaa aaaaaaaaaa 2700 aaaaaaa 2707 <210> SEQ ID NO 263 <211> LENGTH: 2707 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 263 ggcaggccga gccagccgtg cgccgcgctc cagggcccag ggcgccgcac acgcacccac 60 ccacccaccc agcctcgcag cgccatgggc aagaacaagc agccacgcgg ccagcagagg 120 caggggggcc cgccggccgc ggacgccgct gggcccgacg acatggagcc gaagaagggc 180 acgggggccc ccaaggagtg cggggaggag gagccccgga cctgctgcgg ctgccggttc 240 ccgctgctgc tcgccctgct gcagctggcc ctgggcatcg ccgtgaccgt ggtgggcttc 300 ctcatggcga gcatcagctc ctccctgcta gtcagggaca ctccattttg ggctgggatc 360 attgtctgct tagtggccta tcttggcttg tttatgcttt gtgtctcata tcaggttgac 420 gaacggacat gtattcaatt ttctatgaaa ctgttatact ttctgctgag tgccctgggc 480 ctgacggtct gtgtgctggc cgtggccttt gccgcccacc actattcgca gctcacacag 540 tttacctgtg agaccacact cgactcttgc cagtgcaaac tgccctcctc ggagccgctc 600 agcaggacct ttgtttaccg ggatgtgacg gactgtacca gcgtcactgg cactttcaaa 660 ctgttcttac tcatccagat gattcttaat ttggtctgcg gccttgtgtg cttgttggcc 720 tgctttgtga tgtggaaaca taggtaccag gtcttctatg tgggtgtcag gatatgctcc 780 ctcacggctt ccgaaggccc ccagcaaaag atctaacatt cttgctcaaa gttgcgagag 840 aaagtagcac atggagtagc tgaggttaaa caaacaaaaa aaaattttaa acaaagaaag 900 gaaaaaaatt gacaataaaa gtcactcttc taattgaata tttttatatt tttatgaaac 960 aaaagagcat ttcttcaggt ttctattgta ttttttttaa cattcttgca gagaaagcaa 1020 gatccaaatt gattttggga tattaaaagt taacagaaca ctgaacaagg aaagaatggc 1080 atagatctat ctttacagtc tggagttaat tcctgttaac tcattttatc cattccttac 1140 ataatcttct ttcctgttag tccagtttga tggtgtgaat ggtgaatttc aggcccagtt 1200 gctaaatttt gtggcatctt cctctagtcc ttcccacctc cagtcatcag ccccactctg 1260 tcttggagac aggcaggagg tgggggaaga gctgaatctc tttattttcc ctggtagaga 1320 catcttcaag gcatgaaata gcttaaagag cagagtagaa atggaagagg ctttgcaaaa 1380 ggctagataa ctaacaacac ctgggttggg gcggcggcct cttctcttca gctcccttag 1440 cttggctccg taagtggatc acttgccaaa tgctttagat gattgcctct caataattga 1500 aaggtggtgg tagttgtatt ctaaatgatg tagaaggttt aaaaataatt acattatgct 1560 tctattctat catctaaaac aaatcattaa aactaatttc tagctaattg ttaattataa 1620 ttatgctcag aagtctattt aatgagctct gactgtactt acgctgcact gtcggtgtta 1680 agagaaatta ctctcacaag agcagaggcc tgaagattct ttcttctgaa agccaagcac 1740 cacaaggaaa aaaaaattat taatagctca ggttaaaaac acccatttaa acaaaaacaa 1800 gagcatttgt aataggaagt gtttatacaa acagcacatt tgtgatatgt tgaaaagcat 1860 ctctcttggc aaccaatcta tgtttgagga agattgggta atgctgatgt gttccattca 1920 tgaaactgta tttgatacat aatcctatta ttaattcgta tgcttagtca acctaggaaa 1980 tcaaaataat gttttgaagt tcttatttga gcaatatggc cttgacttgg agggtagttt 2040 tagttgtttt gtttttaagt gactgtggtt taaagcacaa atgccccaag gtggggagac 2100 ttctctctgt gattattgtt gctattaaat tctgaactgt atccatattt taaggaagga 2160 gctaaaaatg gaaattcatg aaacataaat ggtatcaaga actttatcag tatgctttgt 2220 tgaaagcaga aattaagata ataattgagt tcaattcgcc tctccgcatt gcctattgat 2280 acactttact aatcatgaaa ttctaaccta aaaggaaaac attttcctgc ttgtcttaga 2340 agaaagtgga ataattccac tgattgtgat aatggtttca atttctacac aatataaata 2400 tccagtataa aggaaagcgt taagtcggta agctagagga ttgtaaatat cttttatgtc 2460 ctctagataa aacacccgat taacagatgt taaacctttt aatgttttga tttgctttaa 2520 aaatggcctt cctacacatt agctccagct aaaaagacac attggagagc ttagaggata 2580 agtctctgga gcagaattta tcacacacaa aagttacacc aacagaatac caagcagaat 2640 gatgaggacc tgtaaaatac cttgtgccct attaaaaaaa aaaaaaaaaa aaaaaaaaaa 2700 aaaaaaa 2707 <210> SEQ ID NO 264 <211> LENGTH: 732 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 264 atgggcaaga acaagcagcc acgcggccag cagaggcagg ggggcccgcc ggccgcggac 60 gccgctgggc ccgacgacat ggagccgaag aagggcacgg gggcccccaa ggagtgcggg 120 gaggaggagc cccggacctg ctgcggctgc cggttcccgc tgctgctcgc cctgctgcag 180 ctggccctgg gcatcgccgt gaccgtggtg ggcttcctca tggcgagcat cagctcctcc 240 ctgctagtca gggacactcc attttgggct gggatcattg tctgcttagt ggcctatctt 300 ggcttgttta tgctttgtgt ctcatatcag gttgacgaac ggacatgtat tcaattttct 360 atgaaactgt tatactttct gctgagtgcc ctgggcctga cggtctgtgt gctggccgtg 420 gcctttgccg cccaccacta ttcgcagctc acacagttta cctgtgagac cacactcgac 480 tcttgccagt gcaaactgcc ctcctcggag ccgctcagca ggacctttgt ttaccgggat 540 gtgacggact gtaccagcgt cactggcact ttcaaactgt tcttactcat ccagatgatt 600 cttaatttgg tctgcggcct tgtgtgcttg ttggcctgct ttgtgatgtg gaaacatagg 660 taccaggtct tctatgtggg tgtcaggata tgctccctca cggcttccga aggcccccag 720 caaaagatct aa 732 <210> SEQ ID NO 265 <211> LENGTH: 681 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 265 atggagccga agaagggcac gggggccccc aaggagtgcg gggaggagga gccccggacc 60 tgctgcggct gccggttccc gctgctgctc gccctgctgc agctggccct gggcatcgcc 120 gtgaccgtgg tgggcttcct catggcgagc atcagctcct ccctgctagt cagggacact 180 ccattttggg ctgggatcat tgtctgctta gtggcctatc ttggcttgtt tatgctttgt 240 gtctcatatc aggttgacga acggacatgt attcaatttt ctatgaaact gttatacttt 300 ctgctgagtg ccctgggcct gacggtctgt gtgctggccg tggcctttgc cgcccaccac 360 tattcgcagc tcacacagtt tacctgtgag accacactcg actcttgcca gtgcaaactg 420 ccctcctcgg agccgctcag caggaccttt gtttaccggg atgtgacgga ctgtaccagc 480 gtcactggca ctttcaaact gttcttactc atccagatga ttcttaattt ggtctgcggc 540 cttgtgtgct tgttggcctg ctttgtgatg tggaaacata ggtaccaggt cttctatgtg 600 ggtgtcagga tatgctccct cacggcttcc gaaggccccc agcaaaagat ctaacattct 660 tgctcaaagt tgcgagagaa a 681 <210> SEQ ID NO 266 <211> LENGTH: 1502 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 266 gtgaatttca ggcccagttg ctaaattttg tggcatcttc ctctagtcct tcccacctcc 60 agtcatcagc cccactctgt cttggagaca ggcaggaggt gggggaagag ctgaatctct 120 ttattttccc tggtagagac atcttcaagg catgaaatag cttaaagagc agagtagaaa 180 cggaagaggc tttgcaaaag gctagataac taacaacacc tgggttgggg cggcggcctc 240 ttctcttcag ctcccttagc ttggctccgt aagtggatca cttgccaaat gctttagatg 300 attgcctctc aataattgaa aggtggtggt agttgtattc taaatgatgt agaaggttta 360 aaaataatta cattatgctt ctattctatc atctaaaaca aatcattaaa actaatttct 420 agctaattgt taattataat tatgctcaga agtctattta atgagctctg actgtactta 480 cgctgcactg tcggtgttaa gagaaattac tctcacaaga gcagaggcct gaagattctt 540 tcttctgaaa gccaagcacc acaaggaaaa acaaattatt aatagctcag gttaaaaaca 600 cccatttaaa caaaaacaag agcatttgta ataggaagtg tttatacaaa tagcacattt 660 gtgatatgtt gaaaagcatc tctcttggca accaatctat gtttgaggaa gattgggtaa 720 tgctgatgtg ttccattcat gaaactgtat ttgatacata atcctattat taattcgtat 780 gcttagtcaa cctaggaaat caaaataatg ttttgaagtt cttatttgag caatatggcc 840 ttgacttgga gggtagtttt agttgttttg tttttaagtg actgtggttt aaagcacaaa 900 tgccccaagg tggggagact tctctctgtg attattgttg ctattaaatt ctgaactgta 960 tccatatttt aaggaaggag ctaaaaatgg aaattcatga aacataaatg gtatcaagaa 1020 ctttatcagt atgctttgtt gaaagcagaa attaagataa taattgagtt caattcgcct 1080 ctccgcattg cctattgata cactttacta atcatgaaat tctaacctaa aaggaaaaca 1140 ttttcctgct tgtcttagaa gaaagtggaa taattccact gattgtgata atggtttcaa 1200 tttctacaca atataaatat ccagtataaa ggaaagcgtt aagtcggtaa gctagaggat 1260 tgtaaatatc ttttatgtcc tctagataaa acacccgatt aacagatgtt aaacctttta 1320 atgttttgat ttgctttaaa aatggccttc ctacacatta gctccagcta aaaagacaca 1380 ttggagagct tagaggataa gtctctggag cagaatttat cacacacaaa agttacacca 1440 acagaatacc aagcagaatg atgaggacct gtaaaatacc ttgtgcccta ttaaaaaaaa 1500 aa 1502 <210> SEQ ID NO 267 <211> LENGTH: 4013 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 267 tgtgtggaac acactcattt ggaggacttt tgtacacata ttttgtagtg tcacatatat 60 gttttaattt tgaattatat ataagggaag gtgggggaag ggcatcatct tctcagagct 120 actttcctct gaacctggaa atgactggaa ctaatattac tttgtgaagt gtccatttac 180 cagaattgtt ctctgtagag agcaactttt gactgtggta atgtaattct tgcactaaga 240 actatgtgta ctagtctcaa aagctgggga ctctgagcct tacctagagt ctcagcaggt 300 ggaccattaa gattaacatt tctagtaggt gagttcaatc acaaaaatat ttcttgttcc 360 atagatttta ttgtggccat gtcagtgaac acccacaagt tttgctcaga atattttagg 420 tgtaagctaa atccctaaat tgttcagagt tcccacagcc ctgtagcagc agagcgagaa 480 ctttaaccag actttttcaa tcccaaagct aatctggagg ccaacagtgt tcaaaacctt 540 ggtgactgag gaaccattta gagttttttc aggctcagga atcacatggt cgttgttggg 600 cttggggtaa gtttcacagg cgatgaagct gacgttgagt cacttgactt ctggagccat 660 aatttatttt ctcccagcaa cctcctactg gggattctca tgtttatgga tacagtttgg 720 caatcactac attgaatgta gtcttttaaa aaaattaact tatgctatta gttgacccat 780 cattgctaat tttggcccac acagtgtttg cattacaaaa acctgttctt tacttcctag 840 tcttgtttca gtcttaatat cagaagttct tgagttcaaa ataagcacaa catgtcatcc 900 agggatggct agcttgtttg ggattcatct aaactgctgg caatatctag acaaaaacat 960 tccacagtcc agctaatatg gttgtcacaa ctcttgaaaa gggcccaaca tctggatggc 1020 aagtgaaaat gtgatcaggg tttaagaact acccactaat aaataaacat ggagctattt 1080 ccatgtcttg ggtgttgtgt ttctaagaag agacagcctt tccatcagaa aatttctggg 1140 agggaagaaa aagaacagtt ttgatgaatt cgctttgcaa atcatcatcc aatgttcttt 1200 gtaaccagaa aggttttctt ctgctttctt gcagctgtta tactttctgc tgagtgccct 1260 gggcctgacg gtctgtgtgc tggccgtggc ctttgccgcc caccactatt cgcagctcac 1320 acagtttacc tgtgagacca cactcgactc ttgccagtgc aaactgccct cctcggagcc 1380 gctcagcagg acctttgttt accgggatgt gacggactgt accagcgtca ctggcacttt 1440 caaactgttc ttactcatcc agatgattct taatttggtc tgcggccttg tgtgcttgtt 1500 ggcctgcttt gtgatgtgga aacataggta ccaggtcttc tatgtgggtg tcaggatatg 1560 ctccctcacg gcttccgaag gcccccagca aaagatctaa cattcttgct caaagttgcg 1620 agagaaagta gcacatggag tagctgaggt taaacaaaca aaaaaaaatt ttaaacaaag 1680 aaaggaaaaa aattgacaat aaaagtcact cttctaattg aatattttta tatttttatg 1740 aaacaaaaga gcatttcttc aggtttctat tgtatttttt ttaacattct tgcagagaaa 1800 gcaagatcca aattgatttt gggatattaa aagttaacag aacactgaac aaggaaagaa 1860 tggcatagat ctatctttac agtctggagt taattcctgt taactcattt tatccattcc 1920 ttacataatc ttctttcctg ttagtccagt ttgatggtgt gaatggtgaa tttcaggccc 1980 agttgctaaa ttttgtggca tcttcctcta gtccttccca cctccagtca tcagccccac 2040 tctgtcttgg agacaggcag gaggtggggg aagagctgaa tctctttatt ttccctggta 2100 gagacatctt caaggcatga aatagcttaa agagcagagt agaaacggaa gaggctttgc 2160 aaaaggctag ataactaaca acacctgggt tggggcggcg gcctcttctc ttcagctccc 2220 ttagcttggc tccgtaagtg gatcacttgc caaatgcttt agatgattgc ctctcaataa 2280 ttgaaaggtg gtggtagttg tattctaaat gatgtagaag gtttaaaaat aattacatta 2340 tgcttctatt ctatcatcta aaacaaatca ttaaaactaa tttctagcta attgttaatt 2400 ataattatgc tcagaagtct atttaatgag ctctgactgt acttacgctg cactgtcggt 2460 gttaagagaa attactctca caagagcaga ggcctgaaga ttctttcttc tgaaagccaa 2520 gcaccacaag gaaaaaaaaa attattaata gctcaggtta aaaacaccca tttaaacaaa 2580 aacaagagca tttgtaatag gaagtgttta tacaaacagc acatttgtga tatgttgaaa 2640 agcatctctc ttggcaacca atctatgttt gaggaagatt gggtaatgct gatgtgttcc 2700 attcatgaaa ctgtatttga tacataatcc tattattaat tcgtatgctt agtcaaccta 2760 ggaaatcaaa ataatgtttt gaagttctta tttgagcaat atggccttga cttggagggt 2820 agttttagtt gttttgtttt taagtgactg tggtttaaag cacaaatgcc ccaaggtggg 2880 gagacttctc tctgtgatta ttgttgctat taaattctga actgtatcca tattttaagg 2940 aaggagctaa aaatggaaat tcatgaaaca taaatggtat caagaacttt atcagtatgc 3000 tttgttgaaa gcagaaatta agataataat tgagttcaat tcgcctctcc gcattgccta 3060 ttgatacact ttactaatca tgaaattcta acctaaaagg aaaacatttt cctgcttgtc 3120 ttagaagaaa gtggaataat tccactgatt gtgataatgg tttcaatttc tacacaatat 3180 aaatatccag tataaaggaa agcgttaagt cggtaagcta gaggattgta aatatctttt 3240 atgtcctcta gataaaacac ccgattaaca gatgttaaac cttttaatgt tttgatttgc 3300 tttaaaaatg gccttcctac acattagctc cagctaaaaa gacacattgg agagcttaga 3360 ggataagtct ctggagcaga atttatcaca cacaaaagtt acaccaacag aataccaagc 3420 agaatgatga ggacctgtaa aataccttgt gccctattaa aaaaaaaaaa aaaaaaaaag 3480 ccagtaactg aatccatttt gatttttggt tgagtttcct acacaaagaa gaaaataact 3540 gagaatctgg aatgttgtag tccatccttt aaagagtaag aaagtagcag ttaatgctag 3600 taaccgtgaa ttaggcacca ctgaaagcac atcccgaatt tctttaacaa caacatttta 3660 tagtgaacac tacaagtttt tatatttaaa aattaagact ctgtatatcc ttaaggtgct 3720 ctatgcttta ccagtaattc acagggtatt tcaaatggta gaatcatttt agcttctgtg 3780 cttccttttt ctaaataatg caacttgtaa gagttgacat tgtaataagc tttataatag 3840 tataaccgtc aggagatata tatatatata tatacacata cacacacaca cacacatata 3900 tactatacat atataaaatg gggatattac tattgtatga ttaaatcatt cttaagtccc 3960 caaggaaaaa aaatcataaa caaatagaaa gaactaaaca gaaaagaaag aaa 4013 <210> SEQ ID NO 268 <211> LENGTH: 4003 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 1,2,3,4,6,7,8,9,10,11, 12,13,14,16,17,266,764,769,773,774, 777,781,783,784,788,789,790,791,792,796, 797,802,808,809,813,814,815,819,820,821, 825,826,830,831,832,833,835,836,839,842, 845,855,856,857,860,861,862,863,867,868, 870,871,877,879,880,881,882,887,892,893, 899,903,904,907,908,910,911,912,913,917, 918,920,921,924,925,926,929,931,933,935, 1011,1012,1015,1023,1026,1081,1098,1133,1136,1137, 3472,3996,4000 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 268 yswktkkwwy wywytywttt ggaggacttt tgtacacata ttttgtagtg tcacatatat 60 gttttaattt tgaattatac ataagggaag gtgggggaag ggcatcatct tctcagagct 120 actttcctct gaacctggaa atgactggaa ctaatattac tttgtgaagt gtccatttac 180 cagaattgtt ctctgtagag agcaactttt gactgtggta atgtaattct tgcactaaga 240 actatgtgta ctagtctcaa aagctkgggg actctgagcc ttacctagag tctcagcagg 300 tggaccatta agattaacat ttctagtagg tgagttcaat cacaaaaata tttcttgttc 360 catagatttt attgtggcca tgtcagtgaa cacccacaag ttttgctcag aatattttag 420 gtgtaagcta aatccctaaa ttgttcagag ttcccacagc cctgtagcag cagagcgaga 480 actttaacca gactttttca atcccaaagc taatctggag gccaacagtg ttcaaaacct 540 tggtgactga ggaaccattt agagtttttt caggctcagg aatcacatgg tcgttgttgg 600 gcttggggta agtttcacag gcgatgaagc tgacgttgag tcacttgact tctggagcca 660 taatttattt tctcccagca acctcctact ggggattctc atgtttatgg atacagtttg 720 gcaatcacta cattgaatgt agtcttttaa aaaaattaac ttakgctakt agyygascca 780 kcmktgckmm kyttgsycca cmcagtgkyt gcmkyacamr maccyrttcy ywmcywccya 840 gyctygtttc agtckymatr ksmaagwwcw wgcagcmamr yrgccarcag akscagggrg 900 gcymgcykgy yksggaykcm kctrrrccyg rcrayatgga gccgaagaag ggcacggggg 960 cccccaagga gtgcggggag gaggagcccc ggacctgctg cggctgccgg kkccmgctgc 1020 tgmtcmgccc tgctgcagct ggccctgggc atcgccgtga ccgtggtggg cttcctcatg 1080 kcgagcatca gctcctcyct gctagtcagg gacactccat tttgggctgg gartcwytgt 1140 ctgcttagtg gcctatcttg gcttgtttat gctttgtgtc tcatatcagg ttgacgaacg 1200 gacatgtatt caattttcta tgaaactgtt atactttctg ctgagtgccc tgggcctgac 1260 ggtctgtgtg ctggccgtgg cctttgccgc ccaccactat tcgcagctca cacagtttac 1320 ctgtgagacc acactcgact cttgccagtg caaactgccc tcctcggagc cgctcagcag 1380 gacctttgtt taccgggatg tgacggactg taccagcgtc actggcactt tcaaactgtt 1440 cttactcatc cagatgattc ttaatttggt ctgcggcctt gtgtgcttgt tggcctgctt 1500 tgtgatgtgg aaacataggt accaggtctt ctatgtgggt gtcaggatat gctccctcac 1560 ggcttccgaa ggcccccagc aaaagatcta acattcttgc tcaaagttgc gagagaaagt 1620 agcacatgga gtagctgagg ttaaacaaac aaaaaaaaat tttaaacaaa gaaaggaaaa 1680 aaattgacaa taaaagtcac tcttctaatt gaatattttt atatttttat gaaacaaaag 1740 agcatttctt caggtttcta ttgtattttt tttaacattc ttgcagagaa agcaagatcc 1800 aaattgattt tgggatatta aaagttaaca gaacactgaa caaggaaaga atggcataga 1860 tctatcttta cagtctggag ttaattcctg ttaactcatt ttatccattc cttacataat 1920 cttctttcct gttagtccag tttgatggtg tgaatggtga atttcaggcc cagttgctaa 1980 attttgtggc atcttcctct agtccttccc acctccagtc atcagcccca ctctgtcttg 2040 gagacaggca ggaggtgggg gaagagctga atctctttat tttccctggt agagacatct 2100 tcaaggcatg aaatagctta aagagcagag tagaaatgga agaggctttg caaaaggcta 2160 gataactaac aacacctggg ttggggcggc ggcctcttct cttcagctcc cttagcttgg 2220 ctccgtaagt ggatcacttg ccaaatgctt tagatgattg cctctcaata attgaaaggt 2280 ggtggtagtt gtattctaaa tgatgtagaa ggtttaaaaa taattacatt atgcttctat 2340 tctatcatct aaaacaaatc attaaaacta atttctagct aattgttaat tataattatg 2400 ctcagaagtc tatttaatga gctctgactg tacttacgct gcactgtcgg tgttaagaga 2460 aattactctc acaagagcag aggcctgaag attctttctt ctgaaagcca agcaccacaa 2520 ggaaaaaaaa attattaata gctcaggtta aaaacaccca tttaaacaaa aacaagagca 2580 tttgtaatag gaagtgttta tacaaacagc acatttgtga tatgttgaaa agcatctctc 2640 ttggcaacca atctatgttt gaggaagatt gggtaatgct gatgtgttcc attcatgaaa 2700 ctgtatttga tacataatcc tattattaat tcgtatgctt agtcaaccta ggaaatcaaa 2760 ataatgtttt gaagttctta tttgagcaat atggccttga cttggagggt agttttagtt 2820 gttttgtttt taagtgactg tggtttaaag cacaaatgcc ccaaggtggg gagacttctc 2880 tctgtgatta ttgttgctat taaattctga actgtatccc atattttaag gaaggagcta 2940 aaaatggaaa ttcatgaaac ataaatggta tcaagaactt tatcagtatg ctttgttgaa 3000 agcagaaatt aagataataa ttgagttcaa ttcgcctctc cgcattgcct attgatacac 3060 tttactaatc atgaaattct aacctaaaag gaaaacattt tcctgcttgt cttagaagaa 3120 agtggaataa ttccactgat tgtgataatg gtttcaattt ctacacaata taaatatcca 3180 gtataaagga aagcgttaag tcggtaagct agaggattgt aaatatcttt tatgtcctct 3240 agataaaaca cccgattaac agatgttaaa ccttttaatg ttttgatttg ctttaaaaat 3300 ggccttccta cacattagct ccagctaaaa agacacattg gagagcttag aggataagtc 3360 tctggagcag aatttatcac acacaaaagt tacaccaaca gaataccaag cagaatgatg 3420 aggacctgta aaataccttg tgccctatta aaaaaaaaaa aaaaaaaaaa arccagtaac 3480 tgaatccatt ttgatttttg gttgagtttc ctacacaaag aagaaaataa ctgagaatct 3540 ggaatgttgt agtccatcct ttaaagagta agaaagtagc agttaatgct agtaaccgtg 3600 aattaggcac cactgaaagc acatcccgaa tttctttaac aacaacattt tatagtgaac 3660 actacaagtt tttatattta aaaattaaga ctctgtatat ccttaaggtg ctctatgctt 3720 taccagtaat tcacagggta tttcaaatgg tagaatcatt ttagcttctg tgcttccttt 3780 ttctaaataa tgcaacttgt aagagttgac attgtaataa gctttataat agtataaccg 3840 tcaggagata tatatatata tatacacata cacacacaca cacacatata tactatacat 3900 atataaaatg gggatattac tattgtatga ttaaatcatt cttaagtccc caaggaaaaa 3960 aaatcataaa caaatagaaa gaactaaaca aaaaaraaar aaa 4003 <210> SEQ ID NO 269 <211> LENGTH: 243 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 269 Met Gly Lys Asn Lys Gln Pro Arg Gly Gln Gln Arg Gln Gly Gly Pro 5 10 15 Pro Ala Ala Asp Ala Ala Gly Pro Asp Asp Met Glu Pro Lys Lys Gly 20 25 30 Thr Gly Ala Pro Lys Glu Cys Gly Glu Glu Glu Pro Arg Thr Cys Cys 35 40 45 Gly Cys Arg Phe Pro Leu Leu Leu Ala Leu Leu Gln Leu Ala Leu Gly 50 55 60 Ile Ala Val Thr Val Val Gly Phe Leu Met Ala Ser Ile Ser Ser Ser 65 70 75 80 Leu Leu Val Arg Asp Thr Pro Phe Trp Ala Gly Ile Ile Val Cys Leu 85 90 95 Val Ala Tyr Leu Gly Leu Phe Met Leu Cys Val Ser Tyr Gln Val Asp 100 105 110 Glu Arg Thr Cys Ile Gln Phe Ser Met Lys Leu Leu Tyr Phe Leu Leu 115 120 125 Ser Ala Leu Gly Leu Thr Val Cys Val Leu Ala Val Ala Phe Ala Ala 130 135 140 His His Tyr Ser Gln Leu Thr Gln Phe Thr Cys Glu Thr Thr Leu Asp 145 150 155 160 Ser Cys Gln Cys Lys Leu Pro Ser Ser Glu Pro Leu Ser Arg Thr Phe 165 170 175 Val Tyr Arg Asp Val Thr Asp Cys Thr Ser Val Thr Gly Thr Phe Lys 180 185 190 Leu Phe Leu Leu Ile Gln Met Ile Leu Asn Leu Val Cys Gly Leu Val 195 200 205 Cys Leu Leu Ala Cys Phe Val Met Trp Lys His Arg Tyr Gln Val Phe 210 215 220 Tyr Val Gly Val Arg Ile Cys Ser Leu Thr Ala Ser Glu Gly Pro Gln 225 230 235 240 Gln Lys Ile <210> SEQ ID NO 270 <211> LENGTH: 243 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 270 Met Gly Lys Asn Lys Gln Pro Arg Gly Gln Gln Arg Gln Gly Gly Pro 5 10 15 Pro Ala Ala Asp Ala Ala Gly Pro Asp Asp Met Glu Pro Lys Lys Gly 20 25 30 Thr Gly Ala Pro Lys Glu Cys Gly Glu Glu Glu Pro Arg Thr Cys Cys 35 40 45 Gly Cys Arg Phe Pro Leu Leu Leu Ala Leu Leu Gln Leu Ala Leu Gly 50 55 60 Ile Ala Val Thr Val Val Gly Phe Leu Met Ala Ser Ile Ser Ser Ser 65 70 75 80 Leu Leu Val Arg Asp Thr Pro Phe Trp Ala Gly Ile Ile Val Cys Leu 85 90 95 Val Ala Tyr Leu Gly Leu Phe Met Leu Cys Val Ser Tyr Gln Val Asp 100 105 110 Glu Arg Thr Cys Ile Gln Phe Ser Met Lys Leu Leu Tyr Phe Leu Leu 115 120 125 Ser Ala Leu Gly Leu Thr Val Cys Val Leu Ala Val Ala Phe Ala Ala 130 135 140 His His Tyr Ser Gln Leu Thr Gln Phe Thr Cys Glu Thr Thr Leu Asp 145 150 155 160 Ser Cys Gln Cys Lys Leu Pro Ser Ser Glu Pro Leu Ser Arg Thr Phe 165 170 175 Val Tyr Arg Asp Val Thr Asp Cys Thr Ser Val Thr Gly Thr Phe Lys 180 185 190 Leu Phe Leu Leu Ile Gln Met Ile Leu Asn Leu Val Cys Gly Leu Val 195 200 205 Cys Leu Leu Ala Cys Phe Val Met Trp Lys His Arg Tyr Gln Val Phe 210 215 220 Tyr Val Gly Val Arg Ile Cys Ser Leu Thr Ala Ser Glu Gly Pro Gln 225 230 235 240 Gln Lys Ile <210> SEQ ID NO 271 <211> LENGTH: 243 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 271 Met Gly Lys Asn Lys Gln Pro Arg Gly Gln Gln Arg Gln Gly Gly Pro 5 10 15 Pro Ala Ala Asp Ala Ala Gly Pro Asp Asp Met Glu Pro Lys Lys Gly 20 25 30 Thr Gly Ala Pro Lys Glu Cys Gly Glu Glu Glu Pro Arg Thr Cys Cys 35 40 45 Gly Cys Arg Phe Pro Leu Leu Leu Ala Leu Leu Gln Leu Ala Leu Gly 50 55 60 Ile Ala Val Thr Val Val Gly Phe Leu Met Ala Ser Ile Ser Ser Ser 65 70 75 80 Leu Leu Val Arg Asp Thr Pro Phe Trp Ala Gly Ile Ile Val Cys Leu 85 90 95 Val Ala Tyr Leu Gly Leu Phe Met Leu Cys Val Ser Tyr Gln Val Asp 100 105 110 Glu Arg Thr Cys Ile Gln Phe Ser Met Lys Leu Leu Tyr Phe Leu Leu 115 120 125 Ser Ala Leu Gly Leu Thr Val Cys Val Leu Ala Val Ala Phe Ala Ala 130 135 140 His His Tyr Ser Gln Leu Thr Gln Phe Thr Cys Glu Thr Thr Leu Asp 145 150 155 160 Ser Cys Gln Cys Lys Leu Pro Ser Ser Glu Pro Leu Ser Arg Thr Phe 165 170 175 Val Tyr Arg Asp Val Thr Asp Cys Thr Ser Val Thr Gly Thr Phe Lys 180 185 190 Leu Phe Leu Leu Ile Gln Met Ile Leu Asn Leu Val Cys Gly Leu Val 195 200 205 Cys Leu Leu Ala Cys Phe Val Met Trp Lys His Arg Tyr Gln Val Phe 210 215 220 Tyr Val Gly Val Arg Ile Cys Ser Leu Thr Ala Ser Glu Gly Pro Gln 225 230 235 240 Gln Lys Ile <210> SEQ ID NO 272 <211> LENGTH: 217 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 272 Met Glu Pro Lys Lys Gly Thr Gly Ala Pro Lys Glu Cys Gly Glu Glu 5 10 15 Glu Pro Arg Thr Cys Cys Gly Cys Arg Phe Pro Leu Leu Leu Ala Leu 20 25 30 Leu Gln Leu Ala Leu Gly Ile Ala Val Thr Val Val Gly Phe Leu Met 35 40 45 Ala Ser Ile Ser Ser Ser Leu Leu Val Arg Asp Thr Pro Phe Trp Ala 50 55 60 Gly Ile Ile Val Cys Leu Val Ala Tyr Leu Gly Leu Phe Met Leu Cys 65 70 75 80 Val Ser Tyr Gln Val Asp Glu Arg Thr Cys Ile Gln Phe Ser Met Lys 85 90 95 Leu Leu Tyr Phe Leu Leu Ser Ala Leu Gly Leu Thr Val Cys Val Leu 100 105 110 Ala Val Ala Phe Ala Ala His His Tyr Ser Gln Leu Thr Gln Phe Thr 115 120 125 Cys Glu Thr Thr Leu Asp Ser Cys Gln Cys Lys Leu Pro Ser Ser Glu 130 135 140 Pro Leu Ser Arg Thr Phe Val Tyr Arg Asp Val Thr Asp Cys Thr Ser 145 150 155 160 Val Thr Gly Thr Phe Lys Leu Phe Leu Leu Ile Gln Met Ile Leu Asn 165 170 175 Leu Val Cys Gly Leu Val Cys Leu Leu Ala Cys Phe Val Met Trp Lys 180 185 190 His Arg Tyr Gln Val Phe Tyr Val Gly Val Arg Ile Cys Ser Leu Thr 195 200 205 Ala Ser Glu Gly Pro Gln Gln Lys Ile 210 215 <210> SEQ ID NO 273 <211> LENGTH: 5738 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 356,357,358,396,627,691,1719,1722,1731,1739, 3019,3228,3702,3946,3960,4004,4014,4015,4019,4024, 4026,4038,4039,4044,4046,4047,4048,4050,4053,4083, 4085,4087,4089,4090,4092,4094,4097,4098,4100,4105, 4108,4322,4935,4937,5401,5514,5519,5531,5532,5534 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 273 atgttgccag aaatatccac cacaagaaaa atcattaagt tccctacttc ccccatcctg 60 gcagaatcat cagaaatgac catcaagacc caaacaagtc ctcctgggtc tacatcagag 120 agtaccttta cattagacac atcaaccact ccctccttgg taataaccca ttcgactatg 180 actcagagat tgccacactc agagataacc actcttgtga gtagaggtgc tggggatgtg 240 ccacggccca gctctctccc tgtggaagaa acaagccctc catcttccca gctgtcttta 300 tctgccatga tctcaccttc tcctgtttct tccacattac cagcaagtag ccactmskct 360 tctgcttctg tgacttcact tctcacacca ggccamgtga agactactga ggtgttggac 420 gcaagtgcag aacctgaaac cagttcacct ccaagtttga gcagcacctc agttgaaata 480 ctggccacct ctgaagtcac cacagatacg gagaaaattc atcctttctc aaacacggca 540 gtaaccaaag ttggaacttc cagttctgga catgaatccc cttcctctgt cctacctgac 600 tcagagacaa ccaaagccac atcggcwatg ggtaccatct ccattatggg ggatacaagt 660 gtttctacat taactcctgc cttatctaac rctaggaaaa ttcagtcaga gccagcttcc 720 tcactgacca ccagattgag ggagaccagc acctctgaag agaccagctt agccacagaa 780 gcaaacactg ttctttctaa agtgtccact ggtgctacta ctgaggtctc caggacagaa 840 gccatctcct ttagcagaac atccatgtca ggccctgagc agtccacaat gtcacaagac 900 atctccatag gaaccatccc caggatttct gcctcctctg tcctgacaga atctgcaaaa 960 atgaccatca caacccaaac aggtccttcg gagtctacac tagaaagtac ccttaatttg 1020 aacacagcaa ccacaccctc ttgggtggaa acccactcta tagtaattca gggatttcca 1080 cacccagaga tgaccacttc catgggcaga ggtcctggag gtgtgtcatg gcctagccct 1140 ccctttgtga aagaaaccag ccctccatcc tccccgctgt ctttacctgc cgtgacctca 1200 cctcatcctg tttccaccac attcctagca catatccccc cctctcccct tcctgtgact 1260 tcactttctc acctctggcc cggcgacaac cacagatatc ttgggtacaa gcacagaacc 1320 tggaaccagt tcatcttcaa gtttgagcac cacctcccat gagagactga ccacttacaa 1380 agacactgca catacagaag ccgtgcatcc ttccacaaac acaggaggga ccaatgtggc 1440 aaccaccagc tctggatata aatcacagtc ctctgtccta gctgactcat ctccaatgtg 1500 taccacctcc accatggggg atacaagtgt tctcacatca actcctgcct tccttgagac 1560 taggaggatt cagacagagc tagcttcctc cctgacccct ggattgaggg agtccagcgg 1620 ctctgaaggg accagctcag gcaccaagat gagcactgtc ctctctaaag tgcccactgg 1680 tgctactact gagatctcca aggaagacgt cacctcggrg arcatccatc hcaggtccyg 1740 ctcaatccac aatatcacca gacatctcca caagaaccgt cagctggttc tctacatccc 1800 ctgtcatgac agaatcagca gaaataacca tgaacaccca tacaagtcct ttaggggcca 1860 caacacaagg caccagtact ttggccacgt caagcacaac ctctttgaca atgacacact 1920 caactatatc tcaaggattt tcacactcac agatgagcac tcttatgagg aggggtcctg 1980 aggatgtatc atggatgagc cctccccttc tggaaaaaac tagaccttcc ttttctctga 2040 tgtcttcacc agccacaact tcaccttctc ctgtttcctc cacattacca gagagcatct 2100 cttcctctcc tcttcctgtg acttcactcc tcacgtctgg cttggcaaaa actacagata 2160 tgttgcacaa aagctcagaa cctgtaacca actcacctgc aaatttgagc agcacctcag 2220 ttgaaatact ggccacctct gaagtcacca cagatacaga gaaaactcat ccttcttcaa 2280 acagaacagt gaccgatgtg gggacctcca gttctggaca tgaatccact tcctttgtcc 2340 tagctgactc acagacatcc aaagtcacat ctccaatggt tattacctcc accatggagg 2400 atacgagtgt ctccacatca actcctggct tttttgagac tagcagaatt cagacagaac 2460 caacatcctc cctgaccctt ggactgagaa agaccagcag ctctgagggg accagcttag 2520 ccacagagat gagcactgtc ctttctggag tgcccactgg tgccactgct gaagtctcca 2580 ggacagaagt cacctcctct agcagaacat ccatctcagg ctttgctcag ctcacagtgt 2640 caccagagac ttccacagaa accatcacca gactccctac ctccagcata atgacagaat 2700 cagcagaaat gatgatcaag acacaaacag atcctcctgg gtctacacca gagagtactc 2760 atactgtgga catatcaaca acacccaact gggtagaaac ccactcgact gtgactcaga 2820 gattttcaca ctcagagatg accactcttg tgagcagaag ccctggtgat atgttatggc 2880 ctagtcaatc ctctgtggaa gaaaccagct ctgcctcttc cctgctgtct ctgcctgcca 2940 cgacctcacc ttctcctgtt tcctctacat tagtagagga tttcccttcc gcttctcttc 3000 ctgtgacttc tcttctcamc cctggcctgg tgataaccac agacaggatg ggcataagca 3060 gagaacctgg aaccagttcc acttcaaatt tgagcagcac ctcccatgag agactgacca 3120 ctttggaaga cactgtagat acagaagaca tgcagccttc cacacacaca gcagtgacca 3180 acgtgaggac ctccatttct ggacatgaat cacaatcttc tgtcctakct gactcagaga 3240 cacccaaagc cacatctcca atgggtacca cctacaccat gggggaaacg agtgtttcca 3300 tatccacttc tgacttcttt gagaccagca gaattcagat agaaccaaca tcctccctga 3360 cttctggatt gagggagacc agcagctctg agaggatcag ctcagccaca gagggaagca 3420 ctgtcctttc tgaagtgccc agtggtgcta ccactgaggt ctccaggaca gaagtgatat 3480 cctctagggg aacatccatg tcagggcctg atcagttcac catatcacca gacatctcta 3540 ctgaagcgat caccaggctt tctacttccc ccattatgac agaatcagca gaaagtgcca 3600 tcactattga gacaggttct cctggggcta catcagaggg taccctcacc ttggacacct 3660 caacaacaac cttttggtca gggacccact caactgcatc tycaggattt tcacactcag 3720 agatgaccac tcttatgagt agaactcctg gagatgtgcc atggccgagc cttccctctg 3780 tggaagaagc cagctctgtc tcttcctcac tgtcttcacc tgccatgacc tcaacttctt 3840 ttttctccac attaccagag agcatctcct cctctcctca tcctgtgact gcacttctca 3900 cccttggccc agtgaagacc acagacatgt tgcgcacaag ctcagracct gaaaccagty 3960 cacctccaaa tttgagcagc acctcagctg aaatattagc cacstctgaa gtcrscaarg 4020 atasakagaa aattcatmmc tccycmmmcr camctgtagt caatgtaggg actgtgattt 4080 atrawcwtmw aycmcckycm tctgwttygg ctgacttagt gacaacaaaa cccacatctc 4140 caatggctac cacctccact ctggggaata caagtgtttc cacatcaact cctgccttcc 4200 cagaaactat gatgacacag ccaacttcct ccctgacttc tggattaagg gagatcagta 4260 cctctcaaga gaccagctca gcaacagaga gaagtgcttc tctttctgga atgcccactg 4320 gygctactac taaggtctcc agaacagaag ccctctcctt aggcagaaca tccaccccag 4380 gtcctgctca atccacaata tcaccagaaa tctccacgga aaccatcact agaatttcta 4440 ctcccctcac cacgacagga tcagcagaaa tgaccatcac ccccaaaaca ggtcattctg 4500 gggcatcctc acaaggtacc tttaccttgg acacatcaag cagagcctcc tggccaggaa 4560 ctcactcagc tgcaactcac agatctccac actcagggat gaccactcct tatgagcaga 4620 ggtcctgagg atgtgtcatg gccaagccgc ccatcagtgg aaaaaactag ccctccatct 4680 tccctggtgt ctttatctgc agtaacctca ccttcgccac tttattccac accatctgag 4740 agtagccact catctcctct ccgggtgact tctcttttca cccctgtcat gatgaagacc 4800 acagacatgt tggacacaag cttggaacct gtgaccactt cacctcccag tatgaatatc 4860 acctcagatg agagtctggc cacttctaaa gccaccatgg agacagaggc aattcagctt 4920 tcagaaaaca cagcwgygac tcagatgggc accatcagtg ctagacaaga attctattcc 4980 tcttatccag gcctcccaga gccatccaaa gtgacatctc cagtggtcac ctcttccacc 5040 ataaaagaca ttgtttctac aaccatacct gcttcctctg agataacaag aattgagatg 5100 gagtcaacat ccaccctgac ccccacacca agggagacca gcacctccca ggagatccac 5160 tcagccacaa agccaagcac tgttccttac aaggcactca ctagtgccac gattgaggac 5220 tccatgacac aagtcatgtc ctctagcaga ggacctagcc ctgatcagtc cacaatgtca 5280 caagacatat ccactgaagt gatcaccagg ctctctacct cccccatcaa gacagaatct 5340 acagaaatga cattaccacc caaacaggtt ctcctggggc tacatcaagg ggtaccctta 5400 kccttggaca cttcaacaac ttttatgtca gggacccact tcaactgcat ctcaaggatt 5460 ttcacactca cagatgaccg ctcttatgag tagactcctg gagatgtgcc atgrctaasc 5520 catccctctg skgmagagcc cgcctctgcc tctttctcac tggcttcacc tgtcttgacc 5580 tcattttttt cgttttttgc ccattcccaa aaacctccac cttttttggt tcctgggcaa 5640 actttttccc tagggctggg gaaacccaaa atgtggggcc aacccagaac tgaaacattc 5700 cccccaatgg acaacctttt tgaaaagggc ccctttgc 5738 <210> SEQ ID NO 274 <211> LENGTH: 1024 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 274 ccccacccga aacacactca gcccttgcac tgacctgcct tctgattgga ggctggttgc 60 ttcggataat gacctccagg accccactgt tggttacagc ctgtttgtat tattcttact 120 gcaactcaag acacctgcag cagggcgtga gaaaaagtaa aagaccagta ttttcacatt 180 gccaggtacc agaaacacag aagactgaca cccgccactt aagtggggcc agggctggtg 240 tctgcccatg ttgccatcct gatgggctgc ttgccacaat gagggatctt cttcaataca 300 tcgcttgctt ctttgccttt ttctctgctg ggtttttgat tgtggccacc tggactgact 360 gttggatggt gaatgctgat gactctctgg aggtgagcac aaaatgccga ggcctctggt 420 gggaatgcgt cacaaatgct tttgatggga ttcgcacctg tgatgagtac gattccatac 480 ttgcggagca tcccttgaag ctggtggtaa ctcgagcgtt gatgattact gcagatattc 540 tagctgggtt tggatttctc accctgctcc ttggtcttga ctgcgtgaaa ttcctccctg 600 atgagccgta cattaaagtc cgcatctgct ttgttgctgg agccacgtta ctaatagcag 660 gtaccccagg aatcattggc tctgtgtggt atgctgttga tgtgtatgtg gaacgttcta 720 ctttggtttt gcacaatata tttcttggta tccaatataa atttggttgg tcctgttggc 780 tcggaatggc tgggtctctg ggttgctttt tggctggagc tgttctcacc tgctgcttat 840 atctttttaa agatgttgga cctgagagaa actatcctta ttccttgagg aaagcctatt 900 cagccgcggg tgtttccatg gccaagtcat actcagcccc tcgcacagag acggccaaaa 960 tgtatgctgt agacacaagg gtgtaaaatg cacgtttcag ggtgtgtttg catatgattt 1020 aatc 1024 <210> SEQ ID NO 275 <211> LENGTH: 1024 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 275 ccccacccga aacacactca gcccttgcac tgacctgcct tctgattgga ggctggttgc 60 ttcggataat gacctccagg accccactgt tggttacagc ctgtttgtat tattcttact 120 gcaactcaag acacctgcag cagggcgtga gaaaaagtaa aagaccagta ttttcacatt 180 gccaggtacc agaaacacag aagactgaca cccgccactt aagtggggcc agggctggtg 240 tctgcccatg ttgccatcct gatgggctgc ttgccacaat gagggatctt cttcaataca 300 tcgcttgctt ctttgccttt ttctctgctg ggtttttgat tgtggccacc tggactgact 360 gttggatggt gaatgctgat gactctctgg aggtgagcac aaaatgccga ggcctctggt 420 gggaatgcgt cacaaatgct tttgatggga ttcgcacctg tgatgagtac gattccatac 480 ttgcggagca tcccttgaag ctggtggtaa ctcgagcgtt gatgattact gcagatattc 540 tagctgggtt tggatttctc accctgctcc ttggtcttga ctgcgtgaaa ttcctccctg 600 atgagccgta cattaaagtc cgcatctgct ttgttgctgg agccacgtta ctaatagcag 660 gtaccccagg aatcattggc tctgtgtggt atgctgttga tgtgtatgtg gaacgttcta 720 ctttggtttt gcacaatata tttcttggta tccaatataa atttggttgg tcctgttggc 780 tcggaatggc tgggtctctg ggttgctttt tggctggagc tgttctcacc tgctgcttat 840 atctttttaa agatgttgga cctgagagaa actatcctta ttccttgagg aaagcctatt 900 cagccgcggg tgtttccatg gccaagtcat actcagcccc tcgcacagag acggccaaaa 960 tgtatgctgt agacacaagg gtgtaaaatg cacgtttcag ggtgtgtttg catatgattt 1020 aatc 1024 <210> SEQ ID NO 276 <211> LENGTH: 24110 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 276 ccccacccga aacacactca gcccttgcac tgacctgcct tctgattgga ggctggttgc 60 ttcggataat gacctccagg accccactgt tggttacagc ctgtttgtat tattcttact 120 gcaactcaag acacctgcag cagggcgtga gaaaaagtaa aagaccagta ttttcacatt 180 gccaggtacc agaaacacag aagactgaca cccgccactt aagtggggcc agggctggtg 240 tctgcccatg ttgccatcct gatgggctgc ttgccacaat gagggatctt cttcaataca 300 tcgcttgctt ctttgccttt ttctctgctg ggtttttgat tgtggccacc tggactgact 360 gttggatggt gaatgctgat gactctctgg aggtaagaag atagcagctt cttttcatga 420 tccaggccag cccaaatttt cgctaagtcc caactgccat gtacaacatt cagtatcttt 480 actaaggcta atgataccaa aaataggcaa catggactat ttattgagtc tttacattat 540 tagctcattt aatcctcata gttaatttat gaggtaggtc ttgttatccc attaaacaga 600 tgaagttact aaatagttcc tccttttttc acaaggataa atttccacaa gggtaattaa 660 gtgatctctg ctactgagac ctccagaaat tcacgtcttc cattgctgca tatatcatat 720 tgagtaacat ttcagtacca cccttttttc taagataaat tttttactct tgatgacagc 780 attaagaata gtgtgataga ctttttttaa ggagtgttaa taatctaaaa cgttgagaaa 840 gaaaatgcaa ggcatgcaaa acctacccaa ttaacatgca agaggaaaaa acattatctt 900 aatgatttcc aagtaaaaga aaaaatgttg agggagaaaa tgtctttcca gtgcatccca 960 atgtacgggg gacaggcatg gatttaaatc ctcccttaaa atgagttgct ctagggaact 1020 gactactatt caaaagatga gtgagtgggt tcacatttga ggattttatt tttctcgctg 1080 gagaagctca gaaagaagta attttgaagt tcaaaaccat tacctgtggc cataggaatc 1140 tgagagaggc agaactgagt aaaaaatcaa atcttcagaa ttagctgctg ttcattaatg 1200 aggcttagga aaacacaggt aagaaaaaga aacaatattt caagagctca aaaaaaggag 1260 tatatagcaa aacaatttgc tttttaatgt gcatcctgaa gggaacaatt taccctagca 1320 aatgctataa tgtcacctct ataaagttta agaaagatac tcgactgagt ttatatattt 1380 ttcttctaat tttctttatt aaactctcaa attggagttc caaatggaaa gtaataatga 1440 ttctattttg ctgtgcatta tttttgctgc tcgctttttc ttgcttttaa tttgcctctg 1500 acttgaacat ggcatttcaa aaccaatgga gttaggaata cctctttaat gctagaaaat 1560 tacatttcca aaaattgtga tagaattgaa ctactgtaaa ggatgtctgc tataagtgag 1620 cccagtgatg cattttatct ggccatgaat atatgcaaag aatgaaataa atgccctttg 1680 aacagtgctc agggaaaagt gcagataaaa cgttctgctg tcattagttt gccattatct 1740 agatggccag tggtaggtga tgaatacaga aatatgttta acttgagcat aattataatt 1800 atgtttttta aaatacaaaa aaatgtaaaa tcccatctag gggcattgtt aaaatatttt 1860 ctaaaacaat ttaaaagtct ttctgcttaa gctgacataa ttgctaactt catttgataa 1920 gaaatagttt tagaaagggt caaaccttgc tgagagagag attgagagtc ctggaattta 1980 aagtgtcttc tttcatttta gtataaccaa ccaatttgcc atctgtccca tgaaagaata 2040 cttctagtta aaacgaatgg aatgagcagt ccaggttaca cacctcaagt aaacccttgc 2100 taaccttgaa aaatagttaa tatttcttag cttccttctt atttcccata cttaaaatgt 2160 attgctataa tattcccaag aagccttcac atttaaagga agaggctggg catggtggct 2220 tatgcctgta atcccaatac tttggaaggc cgaggcgggc agatcacagg tcaagagatt 2280 gagaccatcc tggccgacat agtgaaaccc catctctaac aaaaatacaa aaattagctg 2340 ggtgtggtgg caggggcctg tagtcccagc tactaaggag gctgaggcag gagaatcgct 2400 tgaactaggg aggaggaggt tgcactgagc cgagattgtg ccactgcact ccagcctggc 2460 gacagagcga gactccatct taaaaaagaa gaagaagaag aagaaccctg taacaaatcc 2520 ggctcccttc tctttcaaca atctctttag ttgtcaatat ttttaaagag acaataatct 2580 cttataataa ttgctacttc aacaggccag gatagaaact tatattttcc acaaatttga 2640 aggttctgat gctagctcaa ttgctcttct cttttcttgc cgccatcctc atttatatat 2700 cacctttggt ccatataaca actcacttta tgtttttatt tttatttttt tatagatttg 2760 gtctcacgct gtcacccagg atagagtgta ctggtgtgat catatctcac tgcagattca 2820 aacttctagg ctcaagtcat cctcccacct cagcctccct agtagctagg cctacaggtg 2880 catgtcccca caactggcta attttaaaaa ttttttgtaa gaacaaggac tttctctgtt 2940 ctctaggctg gtctccaact ccaggcctca agtgatcctc ttgcctcggc ctcctaaagt 3000 actgggatta taggagtgaa ccaccacagc agctcacttt aatccattgt tggacaaaag 3060 tcaacgaaac aagtgttttg ttttgttttg attttttaag aaaaaaaagg aataccaata 3120 gacaatttaa ataagaagga gtattatact tttccagttt tttttttttt ttttagtata 3180 tttggatgat gttggcacgg gatttagaag aagagttttg tggttcaatt cagtataaaa 3240 atatatacaa ttatatcata taaaaggaat gatgctactc ctactagaag agacaaagat 3300 aaagcaaaaa ttgctcctgc ctctcaggag tgcacattta atgaggggaa aacaaagata 3360 cacatgaaac tataataaaa agcataaata aattcatatt ttgagcaaga aataaacgaa 3420 gtatcattgg ggaagaaaat atgcgatgat tacttcctat cagggccatc gaagcaggtc 3480 tcatgaaaga aaaggcattt gagcaaagcc ttgaaacgat gtaaagcatt tcaaattgta 3540 gaaatggcag caggggcctt tcagataagg ggacagagtg gcaaaagtgc aaagagagga 3600 gaagctcagg gcttgttaga ggactaaagt gggcaacaca aagaaggagg cagaaaaagc 3660 tcagatattc tttttgccta ccacactcta cctatctcaa atgaagttct tcgtattagg 3720 taaaaatgct aggaaagaaa atagcacaca gaattacgat gtgcacaacc ctacatcagt 3780 gactagaggc cctcagctac catcctgctc ttgtcattat tgattcattt gtgtctctga 3840 gaagactgat agggagaaga gaatttgggt tttgagattt ttcaagcgta tgtttgcatc 3900 ttaaccctta ttaactgcct tctattaagc aagtcacatt tcttgtcttt ggctcagttt 3960 tttcaattgt atagttgaac tcagttgttt ctaaggtcct tttcagtctt tttttttttt 4020 tttttaacat catgtctcca tgactgtctg aaacttcaga gagttggaca ctcactaatg 4080 gactggtggt gtctggcact tctccagaca tttccattgg gaatctagtg gaaggatcct 4140 ccatttttct gtagcttcat acactctccc ttccttcatt ccaacttctc tttttccttc 4200 atttccttgt tccttccttc ctcttcttta ttccccctct ctcttttcct cccttttctt 4260 aactctctct ctttccctcc tatatccttc tttttctttc tttctctttc ttcttcatct 4320 ctttacccct tcatttctct ctcttttctt tctacctttt gtcatttcac aaataatctc 4380 tgacaacttc tgtatacttg gcaccatggt gggtacatgg ttatgaagta ggatgagacc 4440 tggagcctcc ctaggctact gccagtgtag tgagtgggac aaataggtga accgacagtt 4500 atagcaccat gtagcacaca ctatgataat gaaaacccta agcgagtggc tcacttggtc 4560 ttggataacc agtgaaagct acccaaaaga agagatatct aaactaggac ttgaagaaca 4620 ggtgagtgaa gcaggagaag tagagagtat tccaagctca ggaaatggca ggaactgagg 4680 tcaaggtaca agagcgttgt atgtttgcgg tattttgtat atttcatcat agtaagaatt 4740 tccagtttag agaaaagaat acaggggttg ggtcattaag agttttgcat aacatgtaaa 4800 atatagatct tataccatag gcaagggttt gtcgctgtaa gcaatatgta catgtatttt 4860 agaaagatta atcattctgg ctatctgtgg ggagagattg gaagggtaaa atgaggtatg 4920 gggagaacaa ctaggagact tttgttatag accagaaggg agacaatagt ggtctgtact 4980 tcagtgacag caagcatgaa gaaatatgaa ataagggagg ctctaaaaat gtcaaattga 5040 tgagagttat aattgactgc atgtggggaa gtaggtgatg aagagacaca gtcaaagatg 5100 aaatctgcct ttctgatctg gggcaattgg aggggtggtg atgttactca ccaagagttt 5160 aaatgaatga aaattagtat ctatacagaa accttcatgg agcaatgtcc ctgaaccatc 5220 ctactatttt tttctgctta gcttattata caatacttag aggtaggaac acaattcttt 5280 acaatggaga tgtttataga tttaacttta tatcagaggg acctgaggtt aaatcccacc 5340 ttaccaggca gtggctgtat gaatttagac agactcttaa atagctataa accacatttc 5400 ctattcagta atgagagaat aacaatacac acatcataag tttcttgtga gaattaaatg 5460 agcttgtgta tctaaagcat ttgccacagc agcaggcaga tatgaatcag ccaataaata 5520 ttagatacat tattgtctat ttgcagttta ttggtttgtt tttgttctgg agaaggagat 5580 gacattttgc ataatgttcg ctgaacagag aaatataagg tttaaattct attcctattt 5640 ttggtattgc ttctcttgga gaaattttgt ttcctcctct aaagctgtca tttgcctttt 5700 tttttttttt tttttttaaa tcagaatctc tctctgtcgc ccaagctgga gtgcagtggc 5760 atgatcttgg ctcactgcag cctccacctc ctgagttcaa gcgattctcc tgcctcagcc 5820 tcctgagtag ccgggactac aggcaagcac caccacaccc ggctaatttt tttgtatttt 5880 ttgtagagac ggggtttcac catattggcc aggctcgtct tgaactcctg acctcaggtg 5940 atccgcccac ctcatcctcc caaagtgctg ggattacagg tgtgaaccag catggctggc 6000 cacccatttt tatatttaca tctatttcct ttttgtctga ccagggaaat aagacagata 6060 ataagtcaaa tagtgaaggt tatttatcaa atgctcacat ttacaaagaa aataaattga 6120 gataatagca ttgttaatat gttaactaca agatatgcaa ttcttaatta tttacactga 6180 aatagtttct tcacacagta gttactgatc tctcaattat aaaaaggaaa aagtgttttc 6240 acaagaagat ttcattttca gttcatcttt gttaattatt tattgagaac ctgctatgta 6300 ctgagcacta gtatgattaa aattttatta cctcaaaaca aagttgctca cattagtatt 6360 tattttatct gtataatcag gttctcttct gggatttcta tttgcattaa tattacaatt 6420 cttttaaata taaagtaaat attaaaatta ttatatccag catgcccgtt gattatatcc 6480 atttttaaac tttccaattg atttcaaact ctttcagcag atgtttgagg ctacaaatgt 6540 tctcttattt atctcatgat ttcctaagta cctagcactg atgtacatta atgtgaactc 6600 atgatgcatt tgctcacatg agttgataga gcgcctagta acacacttag catacctgtt 6660 gaaagaatga atatattaat gatatgaggt gattattgaa aatctcacat tgaaccttaa 6720 ataagaagta tgtctgtaat gaaatgatca tttttttaaa gcaagatttc gtatcttgct 6780 acaatttaaa tattttcagg atatgtattt ggttcatttt taaaaataaa attggaatac 6840 aaatctgatt cttgggatat ctaataaggt tgatgaagag tatattctgg actagagaat 6900 gtggcttttt gcttagtgct ttaaagagag aaataaagaa aacagagaga aaaaagaaat 6960 tgataatttg taataattta ctcaacataa attgtgatct ttatcactgg gcaataatca 7020 ttacaaagtt gtaatgccat acttttaaaa ggaagacatt ttaacgtatg taaccattta 7080 aaaatgttaa aatgaaaata tttagaaagt tcagatatat aacgtaggtc atatacctgt 7140 gaagagcaca aaattttatt tttctactaa gttggcatta cccatttctt atgatttata 7200 cctttagcca gtgctccaca aataaccaga actaaaacaa ataaatttta gcaaataaag 7260 tcatgttttt ctttcgtatc ttataaatgt aagatataaa gtaaaaagaa aaggcaacat 7320 tgattatgat tattttagtc ttgctccctc atctttatta aggcctgtat tgactccatt 7380 taggccctgg gatagtaaaa aatataatat aaaatgtaaa ggtaaaatgt tcagagtctt 7440 ggttggaaaa tttaaatgca ttttatgtta aaattgaaaa tgtttccaat tttagtagtc 7500 aaacgttatt tactacaata ttattaaaac ttttgcgtct taataaatat aagtaagtac 7560 taagtaggta tctaagtagg aaagtcacat cttcaaggtt aaaatatatt agcacatgga 7620 tagtaaagtg gtgtgaaaat tataaattct tacaatttgt atatgcaagg tggtttttta 7680 aaataatata tcttaatagc ttattttctt ttagttgtct gtacatttat aatcttaatg 7740 catattgaca aaaaataatc ttgatagcgg ttaaccaaca ataaacattt acaaaatctg 7800 ctgtgtatat ttactctctc tctctctctg tagatagata catagataga tagatagata 7860 gacacacaca cagacataat ttcctatgtt actagagaag agataaatgc cgaacattgt 7920 tgaatgtctc taattctcaa gtatttttta gtgtttctaa ttctcaaaag atacataaaa 7980 agacaaggca ggcaaaattg ttgctgctta tatttcaaga ttgataacaa aagagaaact 8040 gggaaaaact aggttagaga agtcttaatg ggagactgct atagagtcca gaataagaaa 8100 tcccaggatt aaggaactaa tttatgtcac tgtaactcaa gttggaagag tcatcatctc 8160 tatggtttcc taacactttt aagtgacatc ctactcattt ttagtactgt ggtaaacact 8220 ttccagagcc agttgagtaa acaaggtcca gaatgacacc aaatcaatgt aagctcttca 8280 gtctaaatca taattttttg gcttctggat ttagctgttt ttgtttattt agtcaagtag 8340 aaattgcact tattaagtag caactgtgca tataataacc attttctgct ccaaacttcc 8400 aatgagagta tatgaattga ttgacaaatt gagattttct tatcctcact aaacatttat 8460 taagcaccta ttatgtatca agagtaagag actgtatgct ccttgaagcc agctgccatg 8520 tttgtcttta ttatcgctgt atctccagca ttaatatagt cggcatgttg actagtaaat 8580 gacaggcatt taataaatat agtttgaaga ataacagatg acctataatt gcacatacaa 8640 aagataatgc aatattttaa atgctataat aatatggaca aattcctgtg ggatttcagg 8700 atagaaagtg ataaatgcca gctagagaga cttgggtggt gggaggctaa tgaaaaaaca 8760 gaagtcttta aaatggggct tgaataataa gtagaagttt gacaggttga gagcaaggag 8820 ttattctcat tagtataatt agtatatacc aggaagagaa aactcaaatg ccttaaggaa 8880 ccaagtagcc agcgttcacg agagaggcag gttgggtagg atctgtgggg aacctggtga 8940 gcctgagctc cacctaaatg ggagcagcca ctcctttctt gccagttgtt gctttgtgag 9000 actggtgagt tcaggtaccc agaatgacca agtttctaag ggaaccctga aatctgaact 9060 gttctgtaaa atctctacac atttttggca actaattaag agattttttg ctttcctcat 9120 gcttgtgact tctactttat tattgtacct taaataaacc tacctctctc catttagcag 9180 gtaatccact cttcactttt gggaacaata gatattcatt gaaacaatac aaattagcat 9240 tgttttaacg ttatttatca atatataagt tgcatgttag aaggagaaat tttaaattta 9300 taatcctcta tttcagacaa ctctgtcaga ttaaaagtta ttacttaaca tttgcatttt 9360 ttacccttta agaaaggtta actatgatat ttgaaacatc agtctgcttt tttaagaacc 9420 ctgtcttaaa attttcaaga atttagattt gcttgctttt tagtttctaa taagccattt 9480 tacaacagag gaataagtaa atgaagatga taaatcatac cagagagcat tcctaaatat 9540 aataaaaaac atgaaaaatt gtaaccttgt cttttgtgca caaaggcacc tttaagggtg 9600 tctccagtga gtgctacatt aacacagaag tttagttaat tacagccact attctcacgt 9660 accttaactg agtgtgaata ccaagccatc taatagtgtg cccctgagca ttaataccta 9720 atgaaattgg attccttgtt ttctctaatg agctcattgc ttttctaaat atggtcattg 9780 caggtaaatg atcaatagcc ttgaaactga taccactact gaattatttt ggcaagatgg 9840 aaatactctt atttgtgtaa aataagaatt tttgaatatg catttcagat cactttctaa 9900 ataatgtcat gtatgacagg aatgaccata gtaggctagt ttgtttcagt ggctggctta 9960 tacagtaaga aattgtggag agtcgctgtc tgatttacag cacagtgcct tcaaacttgt 10020 atcacctagc ttgagctaaa gtgaactgga tgcagcgtgt tcctgttcat taagacacta 10080 cagggcagtc agctttgaga agatctgttt tctgttatga tatagcagtt ctgtacaaac 10140 tgtctctaat atactaattt cctatagttg ccgtaacaaa tgaccataaa ctcggtggct 10200 taacaaaaga taactttatt ctctcacagt tctggaggct ggaagcttat aatcaagaag 10260 ttggcaaggc tgcgctgccc ctgaaagttc tggaagaatc cgttcttagc ctcttccagc 10320 ttctggtggc tgtaggcatt ccttgacttg tagctttatc cctccaatgt ctctgcctca 10380 gaggtcacat tgcatctttc ttttgtctgt ttctctcctg catgtgtctc ttataatgaa 10440 atttgtcagc ccacctgtat aacccaatat gatctcaagg tcctcagtta cattttcaaa 10500 gatccttttt ccaaataagg tcatatactg gtggtaagaa tgtggacata tctttctgag 10560 ggcctccatc tttctccacc ttcactgtgg ttagttagta aagcctaaca cagccactac 10620 tcaagtcatt atgatgttta agcactttac taccactatt tttatttatt gagcatatca 10680 tttatattgc gtgtgtattt gtaattttta attcttataa ccatcctatg attatctccc 10740 gtatacagat aaggagattg aggatcaaaa aaggtaagat cttccccaag gttacaacat 10800 agatagtaag agtttcaatc tatatttaat atttaatgca tatataaatt taatttacgt 10860 gtaatgcaca tataaattta gacgtccaca ttatttagaa atttatatgt tgaatttcac 10920 aagatagctg tttatcatta gattttttga tctctgtgtt acacaggatg agataatcct 10980 ccagaaagtc caagaattgt ttccaactta aacctaagga ggagcatgcc aaggtgaagt 11040 tcgcagaata atagccttgg gatgagatcc aagttagggc ttacttcacc caaagctatc 11100 atccaatacc caattctgga ttactttatt ttaaaatgga tttggaattc tttttaaaaa 11160 aatgttttta ggctgggcac ggtgcctcac gcctgtaatc ccagcacttt gggaggccga 11220 ggtgggcgga tcacctgagg tcaggagttc gagatcagcc tgaccaacat ggggaaaccc 11280 cgtctctact aaaaatactt aaaaaaaaaa agtagcctgg cgtggtggcg catgcctgta 11340 atcccatcta ctcgggaggc tgaggcagga gaatcgcttg aacccagaag gtggaggttg 11400 ccgtgagccg atcgcgccat tgcactccag cctggggaaa acagcgagac tctgcctcaa 11460 aaaaaattgt ttttaaacat ttgtaactgt ttaaacaatt ttttagcaca tatgcatctt 11520 cttaaatggg gtacctagtg atgttttgat acatataatg tatagtgatc ccattagggt 11580 aattagcata cccatcatct caaacattta ttttttgttg gaaacattaa atatcctttt 11640 ttctagctat ttgaaattat atcattatta acaatagcca tcctagagtg ctatagaaca 11700 ggggtccaca acccccaggc cacagaccag tactagtccg tggcctgtta gtaactgggc 11760 tgtgcagtgg gaggtgagca gtgagcaagt gagcattacc gcctaatggt ggacagaagc 11820 tccaccttct gtcggatcag cggcagtatt cgattctcat aggagtgcaa accctgttgt 11880 gaactgcaca tgcgagggtt ctgagttgca tgctccttac aagcacctaa tgcctgatga 11940 tctgagctgg aacagtttca tccaaaagca tccccaaccc cctacccact ggttccatgg 12000 aaaaattgtc ttgcacgaaa ccggtccctg gtgccaaaaa ggttgaagac cactggtata 12060 gaacactgga acttattcct cttatctagc tgcaattttg tatctcttaa caaatctctc 12120 cttgttcctt ggcccctacc cttcccagcc ttcagtatcc tctgtcttat tttttacctc 12180 gaggtttttt tttctgtttg tttgtttaga cggaatctcg ctctgtcgcc aggctgcagt 12240 gcagtggcgc gatctcggct cactgcaaca tccgactcag tggttcaagc gatgctcctg 12300 cctcccgagt ggctgggatt acaggcacgc accaccacgc ctagctaatt tttgtatttt 12360 tagtagagac ggggtttcac catgttagcc aggatgatcc cgatctcctg acctcttgat 12420 ccgtccgcct cagcctccca aagtgctggg attacaggcg tgagccaccg tgcccgaccg 12480 agatcaactt cttatagctt ccacatatga gtaaaaatat gcaatgttta actttctatt 12540 cctggcttat ttcatttaac attattcagt tccatccatg ctgacttaaa taaaagaatt 12600 tcatttttta aattgttaaa tagtattcca ttgtgtagat ataccatatt gtatttaccc 12660 attgctctgt ggttggatat ctaggttgat tccatgtctt ggctattgtg aatagtgtca 12720 caaagagcat ggaggtgcgc acatactgat ttcctttcct ttgaataaat gcccagtagt 12780 gagatttgtt ggatcataaa gaatgggttt taaacacact gcaatgctca ggagcacacc 12840 cacacactgc tgtgtttgag tcctatctcc tccattaact atgctttctt ggggttactt 12900 aactttcctg tgccccaatt tcctcatttg taaaatggat gataaataat atctcttaac 12960 gtcccttaag aaataagaaa aataataata tgctaaatag taactgcttt atggtataga 13020 ctctgtattg aataattatt accaactata agtattttac atataaagta gtaatagagg 13080 taaaacattc agaatcgcga tgaagttgca agcagtagaa ttttatttgg cacataacac 13140 ggcctcaaaa aatagcatgg ggcagagagt ttcatagtgc atgtattcct gaatattatt 13200 ttattttcca aagcaaagtg ttcttatgtt tttttttctc cccacagcaa tttaaccccc 13260 tcctttgcat tcctcatccc accctgctct gttatttatt ctttcttggg gaaaaaatta 13320 agtttttatt ttccaagata attcatagtt aaactttact aaactattcc cagatacaga 13380 aggtaatttg aatccataac tgggtcagag gaaacaattg tattagctct gttccatatg 13440 cgtgagctct atcaagaaca cctgaaacta ttttctgttg gcatgtttac gattctaaga 13500 aatctattgt gacttacggt ttgtagataa agtatgagaa ggttcaggga actggtacct 13560 tctagctcta agtggattct tagagtcatc tgcacatcat ttccaagtaa aaatggatta 13620 cagtcgtcaa gttgtatgaa attaatgctc aatctgctta catcctttac atagcttaag 13680 catttataat atatcattgg agcaataaat aagacttggg gcctttatat attttattta 13740 ttggcatctt ttcatttatt ggttttcttt gctaattatt ttatatttat aaacttcata 13800 tataaagata atatttttct tcatggaact cagtattcgt gataaagaaa caatatatat 13860 ttttaataga ctcaaggtgt caacagttat catctattgt tatatatata tatatttttt 13920 ggtgagtaaa tgtcagcaca gtgacatgaa atgatgtttt tccataacca taactcaatg 13980 gtggaagcag ccacagatat ttaaatatat ttagctctgg ttttatctct tccagacgtg 14040 acttatttct ctacccccac ccttcatgag gaagtggatt catttcctgg cccagaaagg 14100 cttcaattgt cagtgcttaa gggaaaatat tctaatacgc attgtttgtt gtaaatgaag 14160 ttctgatcac atgtgtaacc acttactttg ctatcaaaca caaccaccaa cttctctttt 14220 tgatcaaggg gaactgaact gtgcctgcat gaattgtttc acacggtgtc ttctctaaca 14280 tctaggtgag cacaaaatgc cgaggcctct ggtgggaatg cgtcacaaat gcttttgatg 14340 ggattcgcac ctgtgatgag tacgattcca tacttgcgga gcatccctgt acgtatgcct 14400 tagagctcac tgcttgccag gaagggaaag ggacagaaaa ctgagttcag gtttccattt 14460 tgtgctttgt tttctattgt actatattaa ggttcggtcc agtttgtaat ggttagaaat 14520 tgagctcatc tcggaaatgt gaattgaaat atatacttca gcacattttc tcttttctca 14580 tatatttgta aattcattga gggaaaaata ttatcttatt aatctctgct gtccctcaga 14640 gggccaggca tagtgcttca tactcagcag gcttacagta aatggttttt taatcgaaat 14700 aaactcttta gggtgctgta atttcattat taaactggac gggttagggg gaaagcattt 14760 cagagatgtt ttaagctatg acttagttca aatagaaagt ttacagttat ttcagttgaa 14820 ggttagctaa gaaagagaga gtggcagagg cagaaagagg cagacagcca gagagagaga 14880 catagactat ggggatcagt ggaagaaaaa accaacacat gtgacgcact gttacaggca 14940 atattgaagc tggctccctt atcttcctta cttttagctt taaattatag ttaaagccag 15000 gtgcagtggc tcacacttgt aatcctagca ctttgggagg ccaaggcggg tggatcactg 15060 gaggtcagga gttcgaaacc agcctggcca acatggtgaa accccatccc taataaaatt 15120 accaaaaaaa gttagctcat catggtggtg ggagcctgta gttccagcta gtcaggagac 15180 tgaggcagga gaatcacttg aacccagaag gcagaggtta cagtgagccg agatcacacc 15240 actgcactcc agcctgggag acagagcaag acttcatctc aaaaataaaa taataaataa 15300 ataaattata gttacatgtc agcagagccc atgttgctat gaataaagaa atgtcttaaa 15360 tttaaaaatc ttactgttga ttctctcaat ccttctccat agtgtttatt tgtttattta 15420 taagaacatc gaaccctgct aagaaacatc tgttctgtta tgaaagcaaa gtggttttag 15480 tctctttcaa agcaaatgat gggtgatggc accataaggc aacttctttt ctcaagataa 15540 ataaaaaatt aagcccttgg aatgtgactt ttcccctgaa cctctatttc agtccagagg 15600 aaagcactta aaaacagcag cactctaaaa ttcttcatct gctatttaaa agttgggtgc 15660 gtggaacatt tttaaaaaca tagttcataa ggtctttgtt ttatttttgt taaaaaggat 15720 tttcttaatt ctttttcttt tcccctctct gtgctaacct agttctacct acaaagaaac 15780 actatttgct gaataggaat ggacattttg tctattctaa aaattcatta aaatggattt 15840 taattcataa gctgataaga aaatgaaaaa ttaaaaaaaa tttaaaactt ttaaatactg 15900 ttatatacat ttatgcaaga agaaaatata atcactcata agctcactac gtagagaaaa 15960 ccactgttta tatttaatat gttccttttt catctttgac ctatgtaacc tattaacata 16020 tgggggtaga gaaataagtc acgtctggaa gagataaaac ccatatggcc taatatgtaa 16080 tattggccaa gaagagtcat gatttaaata gctgaaagag aaaatgatct aatttccaga 16140 aattaccttc tacttaatag cacaaactaa ctctccttct tctaaagatc tccttatggc 16200 ttcttctatc ctgaactggc aaaaagaagt cttgaaatat tttattctgc ttccctgtgt 16260 caaattttag ccaattatta tttttaaata aaaaaaaatt aaagtgatta tttattcaat 16320 atttattaag aaatttttgt aggacagata tgctaccttc gattcagcaa tcggctacaa 16380 tatttgtgaa tgagacattt tccagagtag gaggcaaaaa ggaaaacatt tatttagttt 16440 ccactatcta ccaggatgct ctctgctagc ataccaacaa caaaactaag tagtgaactg 16500 tggttaaaca agcaataatg tcaataatct catatttttt agttttatga aaacattagg 16560 ggtacttatg ttcaagttca tacaaagtct gacttttacc ggaggggtgt gttaatgtta 16620 cctacttgtc tgtttttttt gctatgtctc tgtgagttaa tatggttcct tcttctgact 16680 ctgctttaac catatgccct ggtcttccag tgaagctggt ggtaactcga gcgttgatga 16740 ttactgcaga tattctagct gggtttggat ttctcaccct gctccttggt cttgactgcg 16800 tgaaattcct ccctgatgag ccgtacatta aagtccgcat ctgctttgtt gctggagcca 16860 cgttactaat agcaggtacc ggtctggctg gactagcaac aggggtaggg agactctgct 16920 aagggcttga ggtgaaggag agagttgtgc tgaagctgct cattttcgga ttatatgtgg 16980 cttccctttc tagattgaaa aactaaaggt cacttctacc agccctgcat actttagctt 17040 tgaagtcagc taattagtct tttgttaata tctcagaaca aaatatgaag ctctcaggcc 17100 gggtgtggtg gcttatgcct atattcccag cactttggga ggccaaggca ggcagatcac 17160 ttgaggccag gagtttgaaa ccagctggcc atcatggtga aaccctatcc ccactaaaaa 17220 tacaaatcca ggcatggtgg tgcacacctg tagtcccagc tactcggcgg ggctgaggca 17280 ggagaatcgc tcgaacccag gaggcggagg ttgcagtgag cagagatcgc gccactgcac 17340 tccagcctgg gcaacagagc aagactccgt ctcacggaaa aaaaaaaaaa aaaaaaggaa 17400 ataaagaaaa aaaaaagctc taaaactatg ttttggccat ttaaaaagtt acataacttc 17460 aatttttaaa ataatttatc ttgtgattat tactgaagtt aaaatcctaa agtaagcccc 17520 aaacttctac ctccttacct atacccacca ccaccaactc caccaattct ttttaacaat 17580 aaactaacaa ttgtgccaag tcctatgtta aacttgtccc acgtactaac ccatttgttc 17640 ataaatgtaa caataaacag atcatattgt tatcctcact taagatgcag ataaataatt 17700 gaagttctga ggactggtca agcatattta ttagtcaagc atgactaata aacaacatat 17760 caaaaagcac tttaagtagt atttattagt gaaacagcaa aaatgatact ttattcaggt 17820 ctgtcttcaa cttcaaagct tagtcctctt cttttgcaac ataatgtctt cttcttgtct 17880 gttagcagga aaaatcttgt ctgctaacaa agcgaatata agtggcagcc tgaccaggca 17940 gtgtggggta gtacatcgat atggagtttg gaactagaaa cacttgtaga tatgtatgtg 18000 tgatatattc acccgtgtct ctgtttcctg atctgcaaag aggcatgagg ctaaggtagt 18060 aacatgtagc ctgaattgct atggtgaaga tgcaatgtgg gcacagcaaa ctgttagctg 18120 actgcctaac cctttgtatg ctcagaactt gggcctccct gacttttgac acagaaatgt 18180 taagtcaacg tcctaataat cctcagattg tattataaag ttacaaaaat ttagaattct 18240 tcccttctgt aagtcattta tttaattatc ccacctactg acagcataga actttttaat 18300 atacaatgta attcatttaa cagatttaaa cattatttaa tctaattatt tacggctata 18360 taattttgtt cgagaatatt tttgagctat catcagtaaa taacccatct tatgtaaaac 18420 aacaaaacaa atagcattta aaaaataagt cactgaagaa aatcctgata ggaatgactg 18480 aagaaataac taaattgaaa gacaaagcat gtcctaagct ttggaaactt tagaattagt 18540 gtgctataaa atttattttt aaagtctata atctgttttg aaggtttaga aagggaattt 18600 ctaactgaaa actgcagata atggcattat agcaatgcta ttgcaatata tactgcgttt 18660 tctaaaggtt atgtgtttat tatctggctt tttttttttt ttttttttga gatggagtct 18720 cgctctgtcg cccaggctgg agtgcagtgg cgtgatctcg gctcactgca agctccacct 18780 cctgggttca cgccattctc ctgcctcagc ctcccaagta gctgggacta caggcgccca 18840 ccaccacgcc tggctacttt ttgtattttt agtagagaag gggtttcacc atgttggcca 18900 ggatggtctc aatctcttga cctcgtgatc cgcccgcctc ggccccccaa agcgctggga 18960 ttacaggtgt gagccaatgt gcccggccta tctgctcctt cttaaagttc ttacattaaa 19020 caattaggag aagaatacag ttaaatagtg atttaaatag atatcacaga ctatctaggg 19080 aaaaaaatgt aaaatttttt ggagactaca tattttattt tattttttta gatttgggaa 19140 agacaaatat ttctctcatt agacagtaaa acaactctgg aaagtaatct gaagagattg 19200 tttgtgaaca catgcatcta acttagcaca gagtagcaga actttgaaat gaaggaaaag 19260 taggatccag ttatttgggt gttggtgggc aagatcttaa cactaacgtt gatacagctt 19320 caggatatca gtaagcatac atttacaagt aaataactga aaatccaact caagcagact 19380 tagacaacat atagattact gatttcttgt aattgccttc tgctaggcat tgagcatgtg 19440 gagagtacat attttaaaaa cactctttta attcagtgtt ttgtcctcca actcaccaca 19500 tttcttattg catctaggct tcaacatgca atttatacct ttaaaataac aggacactag 19560 tggcgtcatt tcaaaccagt taattgtcag agaggctaag ctgtggagat gtatttaaag 19620 ggaataacat ttcttggtcc attcttatat ggtgtgaggg tagtagataa agatttattt 19680 gaaaataaaa acatttttta cttcaattat ttgtgtttga cctcaagaca ctgaaatcag 19740 tgactttaaa aacagttttc acatgggtgc tgattacgta gctggcatag cttcaaaagg 19800 gggtacaggg agcattaaat acaatgatat ttactcacaa tttaaaaatc attacagaat 19860 gaacatatgc tctatgttgt ttgtgttaga ctacattctt tttctgtttt gtttggtttt 19920 gttttagtat tttcctttat acaatactaa catggcattg gaaagacagg agaatcaaag 19980 aaaaccataa cgatgaattt cgatttacac agataagcac tgtgttattt catttttgca 20040 ttttctttat gtataaactg agataaaatt taaaaaagat acaagatgga aggcaaaagg 20100 aagagacaga agaagtgtcc gaagttcggg ttgcccatga atccatgtta ctgtttttac 20160 ctctctgaat cacgccagcc attttgtgta gtaagcaggt atttttggat ttaaattcag 20220 aaaatgtccc ctattatttg tagcatcctc cctttctttc aggtacccca ggaatcattg 20280 gctctgtgtg gtatgctgtt gatgtgtatg tggaacgttc tactttggtt ttgcacaata 20340 tatttcttgg tatccaatat aaatttggtt ggtcctgttg gctcggaatg gctgggtctc 20400 tgggttgctt tttggctgga gctgttctca cctgctgctt atatcttttt aaaggtaaga 20460 ataaaataaa atagcaaatt tccttgcctc cactatcgtt tttcccaatc cagtggaaac 20520 aaatttcaaa aggaaaaaaa tgttatttat ttgaattcct acctattgcc attaaaaatt 20580 ccaattgttc aagggcaatt gaattgtaat actcaaacat tattacccag ttagttctat 20640 attaattgaa aaataaaatc cacaactaca agcatgtcca atattcaaat gtataatagt 20700 tatcttgatg tattacaatt atacatatat acatatatac acacatatac ataccgtata 20760 tatactatat atgtatatat actatataca tatatataca catatagtat atatactata 20820 tatacatact gtatatatac ccttgtatat atacgtatac atagtacata tgtatacaca 20880 tatacacata tgtatatgca tatatgtata tgtatacata tatgtataat tgtaatacat 20940 caaaataact attgtacatt tgaatattgg acatagttgt agttgtggat tttttcaatt 21000 aatgtaacac taacttggta ataatgtttg agtattgtaa ttcagttgcc cttgaacaat 21060 tggaattttt aatggtaatt ggaattttta atggtaacag gtaggaatac acccatgtat 21120 atgcatgtat atatacacac acgtatatgc atgtatatat gcacacacgt atatgcatgt 21180 atatatgcac acacgtatat gcatgtatat atgcacacat gtatatgtat gtatatatgc 21240 acacatgtat atgtatgtat atatgcacac atgtatatgt atattagaat tatacatata 21300 tgtgtgtcta tatatacaat tataccttta taattgtatg catatatgta gatatacata 21360 taattgtaat acattaaaat aactattata catttgaata ttggacatgg ttgtagttgt 21420 gaattttcta tatatatata ttttgatgta ttacaattat acatgcatat atatcttcac 21480 ccactcaact aaatgtatat ttagtgttaa actgagaagt ggactaagat ccagccaaat 21540 acttcttttt aaagaattta acatgttatg ttgggtttct aaaaatatca cctaaaaaac 21600 taagggaata cctctcctga tgaagaaaaa aaaaataaca ggaaatctac ttggctgaat 21660 tttaaaccta aaagaaactt tcagaatgaa aatcttaaat tgtcttctag gattcttctt 21720 agagttccaa aatgatacct tctttgagta tctatattct tgttcctttt gaggaagaac 21780 atataaaatg gtattttata attttcccaa gttcactgag ttctacttat ttttatattt 21840 ctttcaaaca gatgttggac ctgagagaaa ctatccttat tccttgagga aagcctattc 21900 agccgcgggt gtttccatgg ccaagtcata ctcagcccct cgcacagaga cggccaaaat 21960 gtatgctgta gacacaaggg tgtaaaatgc acgtttcagg gtgtgtttgc atatgattta 22020 atcaatcagt atggttacat tgataaaata gtaagtcaat ccaggaacag ttatttagaa 22080 ttcatattga attaaattaa ttgctagctt aatcaaaatg tttgattctc ctatactttt 22140 tctttctatt actcttatat tttcccgtca ttctctctgc taaccttcca ccttatgcac 22200 acactttccc tatattttaa gataagtctg ctaggatgta gaaatatttg tttgtgattt 22260 ctatatagct attagagatt atgacatagt aatattaaaa tgaaatgata cttaaacaga 22320 aagcaatttc caaagaggcc agggacccta atctttgaag agatgaagaa acttactttt 22380 ctccctggct tttggttcac tttttgtact tttaacaagt gggtgaatta tttgataatt 22440 ttgaggaaga ttattctttt aaattcaaac tagtatgtca atgcctacca ttactctgat 22500 tatattaaaa cagaaaaagg aaataacaac ttcgtatacc agccactggt gagagttaaa 22560 gacaagagct gcccccccac ccccaaatgt caaaggcaaa tgctaaattg atactggagc 22620 tcgtggtgac tttctacctc actaacaaca taagggatct ccatattatt tcaccactat 22680 tctagctttg ctgatatatt gccaaatgat tagactacag aatagttcaa ccagagaatt 22740 tactcattta ttgattaaac atccaaatac tattgtaata tactatgtta aaattcatca 22800 attcaagtgc ccacacacca ctgaatcatc agcaccaagc aatatattag acatatggca 22860 aaattcaaca aatatatttt gatataaata aataaacgtt cacgacttta cttaaaaaat 22920 caatgttgcg gctgggcacg gtagctcgcg tctgtaatcc ccgcactttg ggaggccaag 22980 gcgggtggat cacgaggtca agagacggag accatcctgg ctaacatggt gaaaccctgt 23040 ctctactaaa aatacaaaaa ttagccgggc gtggtggcgg tgcctgtagt cccagctact 23100 cgggaggctg aggcaggaga atcgtttgaa cccaggaggt ggaggttgca gtgagcggag 23160 atcgcaccat tgcactccag tctggcaaca gagcgagact ccatctcaaa aaacaaaaat 23220 aaataaataa ataaatattc ttcataaaat gtgggttttg gggaaaatat agaattacat 23280 atacatttaa cgaagtcgct aatgacattt cattcatatt cataatgtaa ccatcttgaa 23340 tttttttaat tgtagcgatt ttaaaaatgt ttgtaaaatt taatttccag ttttctaatt 23400 acttgtcagt cacattaata acattagtac ctttatggta cccttgcagt acctgaaaag 23460 aatatcaacc tgaaaagaat atcaactcac ccagaaatta gttctttgaa aaaaaagaaa 23520 ttaagttgtg aatttctaaa gaccttgaaa taagtgtttc aaatttaaag aacaaagaat 23580 gatgtgaaaa tgagattatg attcctacta catgaattaa cgtttcgaga ttgctgttta 23640 ttacttccca gagtatcttt aacagtattc tctgaagcag ttccaatcta gttggagaat 23700 taacagcaat tgatttaact atctcatttt tattaactgt aatttacttt aaaaatattt 23760 gcaaatcata ctcattagtt atttgatcat tgttctatgc attttaaaat taattttgtg 23820 ttgttcctct caatatttgt ttttaacatt tattcccatt tttattttat actattgtct 23880 gtcatgcttt atgtattcca ataagtgtct tgaaatcctt gtggggaaag gcaggacaaa 23940 aataattagt taattagatt tgaaaaatgt aatttttcca ttttaaatat ttcatttgta 24000 taagaaaata tttcagagaa ccatgatgat aatggatatg tgtgactgtt ttgaattttt 24060 ttctcaatta aaacattttg tatgtaatgg gaggaatgtc aagatttgtt 24110 <210> SEQ ID NO 277 <211> LENGTH: 3111 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 2411,3089,3090,3091,3092,3094,3095,3098,3099,3100, 3101 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 277 ccccacccga aacacactca gcccttgcac tgacctgcct tctgattgga ggctggttgc 60 ttcggataat gacctccagg accccactgt tggttacagc ctgtttgtat tattcttact 120 gcaactcaag acacctgcag cagggcgtga gaaaaagtaa aagaccagta ttttcacatt 180 gccaggtacc agaaacacag aagactgaca cccgccactt aagtggggcc agggctggtg 240 tctgcccatg ttgccatcct gatgggctgc ttgccacaat gagggatctt cttcaataca 300 tcgcttgctt ctttgccttt ttctctgctg ggtttttgat tgtggccacc tggactgact 360 gttggatggt gaatgctgat gactctctgg aggtgagcac aaaatgccga ggcctctggt 420 gggaatgcgt cacaaatgct tttgatggga ttcgcacctg tgatgagtac gattccatac 480 ttgcggagca tcccttgaag ctggtggtaa ctcgagcgtt gatgattact gcagatattc 540 tagctgggtt tggatttctc accctgctcc ttggtcttga ctgcgtgaaa ttcctccctg 600 atgagccgta cattaaagtc cgcatctgct ttgttgctgg agccacgtta ctaatagcag 660 gtaccccagg aatcattggc tctgtgtggt atgctgttga tgtgtatgtg gaacgttcta 720 ctttggtttt gcacaatata tttcttggta tccaatataa atttggttgg tcctgttggc 780 tcggaatggc tgggtctctg ggttgctttt tggctggagc tgttctcacc tgctgcttat 840 atctttttaa agatgttgga cctgagagaa actatcctta ttccttgagg aaagcctatt 900 cagccgcggg tgtttccatg gccaagtcat actcagcccc tcgcacagag acggccaaaa 960 tgtatgctgt agacacaagg gtgtaaaatg cacgtttcag ggtgtgtttg catatgattt 1020 aatcaatcag tatggttaca ttgataaaat agtaagtcaa tccaggaaca gttatttaga 1080 attcatattg aattaaatta attgctagct taatcaaaat gtttgattct cctatacttt 1140 ttctttctat tactcttata ttttcccgtc attctctctg ctaaccttcc accttatgca 1200 cacactttcc ctatatttta agataagtct gctaggatgt agaaatattt gtttgtgatt 1260 tctatatagc tattagagat tatgacatag taatattaaa atgaaatgat acttaaacag 1320 aaagcaattt ccaaagaggc cagggaccct aatctttgaa gagatgaaga aacttacttt 1380 tctccctggc ttttggttca ctttttgtac ttttaacaag tgggtgaatt atttgataat 1440 tttgaggaag attattcttt taaattcaaa ctagtatgtc aatgcctacc attactctga 1500 ttatattaaa acagaaaaag gaaataacaa cttcgtatac cagccactgg tgagagttaa 1560 agacaagagc tgccccccca cccccaaatg tcaaaggcaa atgctaaatt gatactggag 1620 ctcgtggtga ctttctacct cactaacaac ataagggatc tccatattat ttcaccacta 1680 ttctagcttt gctgatatat tgccaaatga ttagactaca gaatagttca accagagaat 1740 ttactcattt attgattaaa catccaaata ctattgtaat atactatgtt aaaattcatc 1800 aattcaagtg cccacacacc actgaatcat cagcaccaag caatatatta gacatatggc 1860 aaaattcaac aaatatattt tgatataaat aaataaacgt tcacgacttt acttaaaaaa 1920 tcaatgttgc ggctgggcac ggtagctcgc gtctgtaatc cccgcacttt gggaggccaa 1980 ggcgggtgga tcacgaggtc aagagacgga gaccatcctg gctaacatgg tgaaaccctg 2040 tctctactaa aaatacaaaa attagccggg cgtggtggcg gtgcctgtag tcccagctac 2100 tcgggaggct gaggcaggag aatcgtttga acccaggagg tggaggttgc agtgagcgga 2160 gatcgcacca ttgcactcca gtctggcaac agagcgagac tccatctcaa aaaacaaaaa 2220 taaataaata aataaatatt cttcataaaa tgtgggtttt ggggaaaata tagaattaca 2280 tatacattta acgaagtcgc taatgacatt tcattcatat tcataatgta accatcttga 2340 atttttttaa ttgtagcgat tttaaaaatg tttgtaaaat ttaatttcca gttttctaat 2400 tacttgtcag ycacattaat aacattagta cctttatggt acccttgcag tacctgaaaa 2460 gaatatcaac ctgaaaagaa tatcaactca cccagaaatt agttctttga aaaaaaagaa 2520 attaagttgt gaatttctaa agaccttgaa ataagtgttt caaatttaaa gaacaaagaa 2580 tgatgtgaaa atgagattat gattcctact acatgaatta acgtttcgag attgctgttt 2640 attacttccc agagtatctt taacagtatt ctctgaagca gttccaatct agttggagaa 2700 ttaacagcaa ttgatttaac tatctcattt ttattaactg taatttactt taaaaatatt 2760 tgcaaatcat actcattagt tatttgatca ttgttctatg cattttaaaa ttaattttgt 2820 gttgttcctc tcaatatttg tttttaacat ttattcccat ttttatttta tactattgtc 2880 tgtcatgctt tatgtattcc aataagtgtc ttgaaatcct tgtggggaaa ggcaggacaa 2940 aaataattag ttaattagat ttgaaaaatg taatttttcc attttaaata tttcatttgt 3000 ataagaaaat atttcagaga accatgatga taatggatat gtgtgactgt tttgaatttt 3060 tttctcaatt aaaacatttt gtatgtaawr rrarraawrw maagatttgt t 3111 <210> SEQ ID NO 278 <211> LENGTH: 305 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 278 Met Thr Ser Arg Thr Pro Leu Leu Val Thr Ala Cys Leu Tyr Tyr Ser 5 10 15 Tyr Cys Asn Ser Arg His Leu Gln Gln Gly Val Arg Lys Ser Lys Arg 20 25 30 Pro Val Phe Ser His Cys Gln Val Pro Glu Thr Gln Lys Thr Asp Thr 35 40 45 Arg His Leu Ser Gly Ala Arg Ala Gly Val Cys Pro Cys Cys His Pro 50 55 60 Asp Gly Leu Leu Ala Thr Met Arg Asp Leu Leu Gln Tyr Ile Ala Cys 65 70 75 80 Phe Phe Ala Phe Phe Ser Ala Gly Phe Leu Ile Val Ala Thr Trp Thr 85 90 95 Asp Cys Trp Met Val Asn Ala Asp Asp Ser Leu Glu Val Ser Thr Lys 100 105 110 Cys Arg Gly Leu Trp Trp Glu Cys Val Thr Asn Ala Phe Asp Gly Ile 115 120 125 Arg Thr Cys Asp Glu Tyr Asp Ser Ile Leu Ala Glu His Pro Leu Lys 130 135 140 Leu Val Val Thr Arg Ala Leu Met Ile Thr Ala Asp Ile Leu Ala Gly 145 150 155 160 Phe Gly Phe Leu Thr Leu Leu Leu Gly Leu Asp Cys Val Lys Phe Leu 165 170 175 Pro Asp Glu Pro Tyr Ile Lys Val Arg Ile Cys Phe Val Ala Gly Ala 180 185 190 Thr Leu Leu Ile Ala Gly Thr Pro Gly Ile Ile Gly Ser Val Trp Tyr 195 200 205 Ala Val Asp Val Tyr Val Glu Arg Ser Thr Leu Val Leu His Asn Ile 210 215 220 Phe Leu Gly Ile Gln Tyr Lys Phe Gly Trp Ser Cys Trp Leu Gly Met 225 230 235 240 Ala Gly Ser Leu Gly Cys Phe Leu Ala Gly Ala Val Leu Thr Cys Cys 245 250 255 Leu Tyr Leu Phe Lys Asp Val Gly Pro Glu Arg Asn Tyr Pro Tyr Ser 260 265 270 Leu Arg Lys Ala Tyr Ser Ala Ala Gly Val Ser Met Ala Lys Ser Tyr 275 280 285 Ser Ala Pro Arg Thr Glu Thr Ala Lys Met Tyr Ala Val Asp Thr Arg 290 295 300 Val 305 <210> SEQ ID NO 279 <211> LENGTH: 305 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 279 Met Thr Ser Arg Thr Pro Leu Leu Val Thr Ala Cys Leu Tyr Tyr Ser 5 10 15 Tyr Cys Asn Ser Arg His Leu Gln Gln Gly Val Arg Lys Ser Lys Arg 20 25 30 Pro Val Phe Ser His Cys Gln Val Pro Glu Thr Gln Lys Thr Asp Thr 35 40 45 Arg His Leu Ser Gly Ala Arg Ala Gly Val Cys Pro Cys Cys His Pro 50 55 60 Asp Gly Leu Leu Ala Thr Met Arg Asp Leu Leu Gln Tyr Ile Ala Cys 65 70 75 80 Phe Phe Ala Phe Phe Ser Ala Gly Phe Leu Ile Val Ala Thr Trp Thr 85 90 95 Asp Cys Trp Met Val Asn Ala Asp Asp Ser Leu Glu Val Ser Thr Lys 100 105 110 Cys Arg Gly Leu Trp Trp Glu Cys Val Thr Asn Ala Phe Asp Gly Ile 115 120 125 Arg Thr Cys Asp Glu Tyr Asp Ser Ile Leu Ala Glu His Pro Leu Lys 130 135 140 Leu Val Val Thr Arg Ala Leu Met Ile Thr Ala Asp Ile Leu Ala Gly 145 150 155 160 Phe Gly Phe Leu Thr Leu Leu Leu Gly Leu Asp Cys Val Lys Phe Leu 165 170 175 Pro Asp Glu Pro Tyr Ile Lys Val Arg Ile Cys Phe Val Ala Gly Ala 180 185 190 Thr Leu Leu Ile Ala Gly Thr Pro Gly Ile Ile Gly Ser Val Trp Tyr 195 200 205 Ala Val Asp Val Tyr Val Glu Arg Ser Thr Leu Val Leu His Asn Ile 210 215 220 Phe Leu Gly Ile Gln Tyr Lys Phe Gly Trp Ser Cys Trp Leu Gly Met 225 230 235 240 Ala Gly Ser Leu Gly Cys Phe Leu Ala Gly Ala Val Leu Thr Cys Cys 245 250 255 Leu Tyr Leu Phe Lys Asp Val Gly Pro Glu Arg Asn Tyr Pro Tyr Ser 260 265 270 Leu Arg Lys Ala Tyr Ser Ala Ala Gly Val Ser Met Ala Lys Ser Tyr 275 280 285 Ser Ala Pro Arg Thr Glu Thr Ala Lys Met Tyr Ala Val Asp Thr Arg 290 295 300 Val 305 <210> SEQ ID NO 280 <211> LENGTH: 305 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 280 Met Thr Ser Arg Thr Pro Leu Leu Val Thr Ala Cys Leu Tyr Tyr Ser 5 10 15 Tyr Cys Asn Ser Arg His Leu Gln Gln Gly Val Arg Lys Ser Lys Arg 20 25 30 Pro Val Phe Ser His Cys Gln Val Pro Glu Thr Gln Lys Thr Asp Thr 35 40 45 Arg His Leu Ser Gly Ala Arg Ala Gly Val Cys Pro Cys Cys His Pro 50 55 60 Asp Gly Leu Leu Ala Thr Met Arg Asp Leu Leu Gln Tyr Ile Ala Cys 65 70 75 80 Phe Phe Ala Phe Phe Ser Ala Gly Phe Leu Ile Val Ala Thr Trp Thr 85 90 95 Asp Cys Trp Met Val Asn Ala Asp Asp Ser Leu Glu Val Ser Thr Lys 100 105 110 Cys Arg Gly Leu Trp Trp Glu Cys Val Thr Asn Ala Phe Asp Gly Ile 115 120 125 Arg Thr Cys Asp Glu Tyr Asp Ser Ile Leu Ala Glu His Pro Leu Lys 130 135 140 Leu Val Val Thr Arg Ala Leu Met Ile Thr Ala Asp Ile Leu Ala Gly 145 150 155 160 Phe Gly Phe Leu Thr Leu Leu Leu Gly Leu Asp Cys Val Lys Phe Leu 165 170 175 Pro Asp Glu Pro Tyr Ile Lys Val Arg Ile Cys Phe Val Ala Gly Ala 180 185 190 Thr Leu Leu Ile Ala Gly Thr Pro Gly Ile Ile Gly Ser Val Trp Tyr 195 200 205 Ala Val Asp Val Tyr Val Glu Arg Ser Thr Leu Val Leu His Asn Ile 210 215 220 Phe Leu Gly Ile Gln Tyr Lys Phe Gly Trp Ser Cys Trp Leu Gly Met 225 230 235 240 Ala Gly Ser Leu Gly Cys Phe Leu Ala Gly Ala Val Leu Thr Cys Cys 245 250 255 Leu Tyr Leu Phe Lys Asp Val Gly Pro Glu Arg Asn Tyr Pro Tyr Ser 260 265 270 Leu Arg Lys Ala Tyr Ser Ala Ala Gly Val Ser Met Ala Lys Ser Tyr 275 280 285 Ser Ala Pro Arg Thr Glu Thr Ala Lys Met Tyr Ala Val Asp Thr Arg 290 295 300 Val 305 <210> SEQ ID NO 281 <211> LENGTH: 58 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 281 Met Ile Arg Leu Gln Asn Ser Ser Thr Arg Glu Phe Thr His Leu Leu 5 10 15 Ile Lys His Pro Asn Thr Ile Val Ile Tyr Tyr Val Lys Ile His Gln 20 25 30 Phe Lys Cys Pro His Thr Thr Glu Ser Ser Ala Pro Ser Asn Ile Leu 35 40 45 Asp Ile Trp Gln Asn Ser Thr Asn Ile Phe 50 55 <210> SEQ ID NO 282 <211> LENGTH: 75 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 282 Met Asn Met Asn Glu Met Ser Leu Ala Thr Ser Leu Asn Val Tyr Val 5 10 15 Ile Leu Tyr Phe Pro Gln Asn Pro His Phe Met Lys Asn Ile Tyr Leu 20 25 30 Phe Ile Tyr Phe Cys Phe Leu Arg Trp Ser Leu Ala Leu Leu Pro Asp 35 40 45 Trp Ser Ala Met Val Arg Ser Pro Leu Thr Ala Thr Ser Thr Ser Trp 50 55 60 Val Gln Thr Ile Leu Leu Pro Gln Pro Pro Glu 65 70 75 <210> SEQ ID NO 283 <211> LENGTH: 414 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <400> SEQUENCE: 283 atgcagcatc accaccatca ccaccacttc ttgcttccag gctttgcgct gcaaatccag 60 tgctaccagt gtgaagaatt ccagctgaac aacgactgct cctcccccga gttcattgtg 120 aattgcacgg tgaacgttca agacatgtgt cagaaagaag tgatggagca aagtgccggg 180 atcatgtacc gcaagtcctg tgcatcatca gcggcctgtc tcatcgcctc tgccgggtac 240 cagtccttct gctccccagg gaaactgaac tcagtttgca tcagctgctg caacacccct 300 ctttgtaacg ggccaaggcc caagaaaagg ggaagttctg cctcggccct caggccaggg 360 ctccgcacca ccatcctgtt cctcaaatta gccctcttct cggcacactg ctga 414 <210> SEQ ID NO 284 <211> LENGTH: 137 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 284 Met Gln His His His His His His His Phe Leu Leu Pro Gly Phe Ala 5 10 15 Leu Gln Ile Gln Cys Tyr Gln Cys Glu Glu Phe Gln Leu Asn Asn Asp 20 25 30 Cys Ser Ser Pro Glu Phe Ile Val Asn Cys Thr Val Asn Val Gln Asp 35 40 45 Met Cys Gln Lys Glu Val Met Glu Gln Ser Ala Gly Ile Met Tyr Arg 50 55 60 Lys Ser Cys Ala Ser Ser Ala Ala Cys Leu Ile Ala Ser Ala Gly Tyr 65 70 75 80 Gln Ser Phe Cys Ser Pro Gly Lys Leu Asn Ser Val Cys Ile Ser Cys 85 90 95 Cys Asn Thr Pro Leu Cys Asn Gly Pro Arg Pro Lys Lys Arg Gly Ser 100 105 110 Ser Ala Ser Ala Leu Arg Pro Gly Leu Arg Thr Thr Ile Leu Phe Leu 115 120 125 Lys Leu Ala Leu Phe Ser Ala His Cys 130 135 <210> SEQ ID NO 285 <211> LENGTH: 1740 <212> TYPE: DNA <213> ORGANISM: Homo sapiens <220> FEATURE: <221> NAME/KEY: misc_feature <222> LOCATION: 755,756,757,758,759,760,761,762,763,764, 765,766,767,768,769,770,771,772,773,774, 775,776,777,778,779,780,781,782,783,784, 785,786,787,788,789,790,791,792,793,794, 795,796,797,798,799,800,801,802,803,804, 805,806,807,808,809,810,811,812,813,814, 815,816,817,818,819,820,821,822,823,824, 825,826,827,828,829,830,831,832,833,834, 835,1605,1606,1607,1608,1609,1610,1611,1612,1613, 1614,1615,1616,1617,1618,1619,1620,1621,1622,1623, 1624,1625,1626,1629 <223> OTHER INFORMATION: n = A,T,C or G <400> SEQUENCE: 285 ggaaaattca tgaagagggg actgaaatcc acaactcaat cagcatagag cagaagtaag 60 ggggaagtgg taagaggtgc actatgaatg agctggagaa tttaaaggga ggctgaactc 120 agagtcgaag tgaccttgag aagataaacc ctctggaaat tctcagaatc tcaggatggg 180 ccccagagta tctaaagatg ctacagttca agggattgag ccaattgtat ataaatctta 240 atggataggt tgacctcagc ataaaacttg ggtggaaatt ttaaacaggt ttctttattt 300 cagcacttct cagagccact cattgtataa ggtactttgt gaatatccag atagtattct 360 tcaaactctc ttttatttcc ccagggggca tcccatagga caagaagcat tctttgtgac 420 actctgtggg aagagctggt ttaaaggggt acctgtctgg gcaacactgt cccacagggg 480 cccccatgac caaactaact ctgcttctac ccagaaaggg tgcagagtag ccactagact 540 tttatgtggc aaatgggatg gttatgccca gcctgaagcc aagatgccct ttctggttgc 600 cttgatttgt gtttaacagc tccaaatgct taatgaggca gtaagagacg tctctcttgg 660 gcagtacttc ccaactaggg gtgagtttgc cacccttacc cccatcccag tgaatatttg 720 caattcctaa agacgtgttt tgattgtcac actgnnnnnn nnnnnnnnnn nnnnnnnnnn 780 nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnacaaa 840 agagaattat ctagccccaa atgtccataa cactgctgtt gagaaaacct accgcaggat 900 cttactgggc ttcataggta agcttgccct ttgttctggc ttctgtagat atataaaata 960 aagacactgc ccagtccctc cctcaacgtc ccgagccagg gctcaaggca aattccaata 1020 acagtagaat gaacactaaa tattgatttc aaaatctcag caactagaag aatgaccaac 1080 catcctggtt ggcctgggac tgtcctagtt ttagcattga aagtttcagg ttccaggaaa 1140 gccctcaggc ctgggctgct ggtcacccta gcagctgagg gactcttcaa tacagaatta 1200 gtctttgcgc actggagatg aatatacttt aatttgtaac atgtgaaaac atctataaac 1260 atctactgga agcctgttct gtctgcaccg acattttcat tgaagtacgg attcttcctg 1320 acctagatga cagctggctg ctgacaactt tgcgagggct cggtatataa actgagcttt 1380 gtacctattt ttaataatta catgatatag tatataactt ggattaaccc agtattcggg 1440 tattttcaat ttccttgggg agcttagagg gacggacaaa taaaaaagat tatttcaaca 1500 ttcaaatata tgccattggt ttacatatga agataaccac atatatgtat aaattcaccg 1560 ttacttttta gcaatactat aaaatccaac agaaaaaaat agcannnnnn nnnnnnnnnn 1620 nnnnnngant tagtctttgt gggtttgggg caagcaactg cccttctcag ttaggatggg 1680 ggagttctgg acatttctag ctaaagccca ggggtcaagg gaatgataaa ctcctcggtc 1740 <210> SEQ ID NO 286 <211> LENGTH: 116 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 286 Met Phe Ile Asp Val Phe Thr Cys Tyr Lys Leu Lys Tyr Ile His Leu 5 10 15 Gln Cys Ala Lys Thr Asn Ser Val Leu Lys Ser Pro Ser Ala Ala Arg 20 25 30 Val Thr Ser Ser Pro Gly Leu Arg Ala Phe Leu Glu Pro Glu Thr Phe 35 40 45 Asn Ala Lys Thr Arg Thr Val Pro Gly Gln Pro Gly Trp Leu Val Ile 50 55 60 Leu Leu Val Ala Glu Ile Leu Lys Ser Ile Phe Ser Val His Ser Thr 65 70 75 80 Val Ile Gly Ile Cys Leu Glu Pro Trp Leu Gly Thr Leu Arg Glu Gly 85 90 95 Leu Gly Ser Val Phe Ile Leu Tyr Ile Tyr Arg Ser Gln Asn Lys Gly 100 105 110 Gln Ala Tyr Leu 115 <210> SEQ ID NO 287 <211> LENGTH: 32 <212> TYPE: DNA <213> ORGANISM: Artificial Sequence <220> FEATURE: <223> OTHER INFORMATION: PCR primer <400> SEQUENCE: 287 cacttcttgc ttccaggctt tgcgctgcaa at 32 <210> SEQ ID NO 288 <211> LENGTH: 29 <212> TYPE: DNA <213> ORGANISM: Artificial Sequence <220> FEATURE: <223> OTHER INFORMATION: PCR primer <400> SEQUENCE: 288 actagctcga gtcagcagtg tgccgagaa 29 <210> SEQ ID NO 289 <211> LENGTH: 114 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 289 Met Trp Val Leu Gly Ile Ala Ala Thr Phe Cys Gly Leu Phe Leu Leu 1 5 10 15 Pro Gly Phe Ala Leu Gln Ile Gln Cys Tyr Gln Cys Glu Glu Phe Gln 20 25 30 Leu Asn Asn Asp Cys Ser Ser Pro Glu Phe Ile Val Asn Cys Thr Val 35 40 45 Asn Val Gln Asp Met Cys Gln Lys Glu Val Met Glu Gln Ser Ala Gly 50 55 60 Ile Met Tyr Arg Lys Ser Cys Ala Ser Ser Ala Ala Cys Leu Ile Ala 65 70 75 80 Ser Ala Gly Tyr Gln Ser Phe Cys Ser Pro Gly Lys Leu Asn Ser Val 85 90 95 Cys Ile Ser Cys Cys Asn Thr Pro Leu Cys Asn Gly Pro Arg Pro Lys 100 105 110 Lys Arg <210> SEQ ID NO 290 <211> LENGTH: 115 <212> TYPE: PRT <213> ORGANISM: Homo sapiens <400> SEQUENCE: 290 Met Trp Val Leu Gly Ile Ala Ala Thr Phe Cys Gly Leu Phe Leu Leu 1 5 10 15 Pro Gly Phe Ala Leu Gln Ile Gln Cys Tyr Gln Cys Glu Glu Phe Gln 20 25 30 Leu Asn Asn Asp Cys Ser Ser Pro Glu Phe Ile Val Asn Cys Thr Val 35 40 45 Asn Val Gln Asp Met Cys Gln Lys Glu Val Met Glu Gln Ser Ala Gly 50 55 60 Ile Met Tyr Arg Lys Ser Cys Ala Ser Ser Ala Ala Cys Leu Ile Ala 65 70 75 80 Ser Ala Gly Tyr Gln Ser Phe Cys Ser Pro Gly Lys Leu Asn Ser Val 85 90 95 Cys Ile Ser Cys Cys Asn Thr Pro Leu Cys Asn Gly Pro Arg Pro Lys 100 105 110 Lys Arg Gly 115 <210> SEQ ID NO 291 <211> LENGTH: 30 <212> TYPE: PRT <213> ORGANISM: Artificial Sequence <220> FEATURE: <223> OTHER INFORMATION: Synthetic peptide used for generation of rabbit polyclonal anti-sera against O591s. <400> SEQUENCE: 291 Tyr Gln Cys Glu Glu Phe Gln Leu Asn Asn Asp Cys Ser Ser Pro Glu 1 5 10 15 Phe Ile Val Asn Cys Thr Val Asn Val Gln Asp Met Cys Gln 20 25 30 <210> SEQ ID NO 292 <211> LENGTH: 25 <212> TYPE: PRT <213> ORGANISM: Artificial Sequence <220> FEATURE: <223> OTHER INFORMATION: Synthetic peptide used for generation of rabbit polyclonal anti-sera against O591s. <400> SEQUENCE: 292 Cys Gln Lys Glu Val Met Glu Gln Ser Ala Gly Ile Met Tyr Arg Lys 1 5 10 15 Ser Cys Ala Ser Ser Ala Ala Cys Leu 20 25 <210> SEQ ID NO 293 <211> LENGTH: 30 <212> TYPE: PRT <213> ORGANISM: Artificial Sequence <220> FEATURE: <223> OTHER INFORMATION: Synthetic peptide used for generation of rabbit polyclonal anti-sera against O591s. <400> SEQUENCE: 293 Thr Pro Leu Cys Asn Gly Pro Arg Pro Lys Lys Arg Gly Ser Ser Ala 1 5 10 15 Ser Ala Leu Arg Pro Gly Leu Arg Thr Thr Ile Gly Cys Gly 20 25 30 

What is claimed:
 1. An isolated polynucleotide comprising a sequence selected from the group consisting of: (a) SEQ ID NO:214; (b) the complement SEQ ID NO:214; (c) a sequence consisting of at least 20 contiguous residues of SEQ ID NO:214; (d) sequences that hybridize to a SEQ ID NO:214 under moderately stringent conditions; (e) a sequence having at least 75% identity to SEQ ID NO:214; (f) a sequence having at least 90% identity SEQ ID NO:214 and (g) a degenerate variant of SEQ ID NO:214.
 2. An isolated polypeptide comprising an amino acid sequence of an ovarian tumor protein selected from the group consisting of: (a) polynucleotides recited in any one of sequences encoded by a polynucleotide of claim 1; (b) sequences having at least 70% identity to a sequence encoded by a polynucleotide of claim 1; (c) sequences having at least 90% identity to a sequence encoded by a polynucleotide of claim 1; (d) sequences provided in SEQ ID NOS: 289-293; (e) sequences having at least 70% identity to a sequence provided in SEQ ID NOS: 289-293; and (f) sequences having at least 90% identity to a sequence provided in SEQ ID NOS: 289-293.
 3. An expression vector comprising a polynucleotide of claim 1 operably linked to an expression control sequence.
 4. A host cell transformed or transfected with an expression vector according to claim
 3. 5. An isolated antibody, or antigen-binding fragment thereof, that specifically binds to a polypeptide of claim
 2. 6. A method for detecting the presence of an ovarian cancer in a patient, comprising the steps of: (a) obtaining a biological sample from the patient; (b) contacting the biological sample with a binding agent that binds to a polypeptide of claim 2; (c) detecting in the sample an amount of polypeptide that binds to the binding agent; and (d) comparing the amount of polypeptide to a predetermined cut-off value and therefrom determining the presence of a cancer in the patient.
 7. A fusion protein comprising at least one polypeptide according to claim
 2. 8. An oligonucleotide that hybridizes to SEQ ID NO:214 under moderately stringent conditions.
 9. A method for stimulating and/or expanding T cells specific for a tumor protein, comprising contacting T cells with at least one component selected from the group consisting of: (a) polypeptides according to claim 2; (b) polynucleotides according to claim 1; and (c) antigen-presenting cells that express a polypeptide according to claim 1, under conditions and for a time sufficient to permit the stimulation and/or expansion of T cells.
 10. An isolated T cell population, comprising T cells prepared according to the method of claim
 9. 11. A composition comprising a first component selected from the group consisting of physiologically acceptable carriers and immunostimulants, and a second component selected from the group consisting of: (a) polypeptides according to claim 2; (b) polynucleotides according to claim 1; (c) antibodies according to claim 5; (d) fusion proteins according to claim 7; and (e) antigen presenting cells that express a polypeptide according to claim
 2. 12. A method for stimulating an immune response in a patient, comprising administering to the patient a composition of claim
 11. 13. A method for the treatment of a cancer in a patient, comprising administering to the patient a composition of claim
 11. 14. A method for determining the presence of a cancer in a patient, comprising the steps of: (a) obtaining a biological sample from the patient; (b) contacting the biological sample with an oligonucleotide according to claim 8; (c) detecting in the sample an amount of a polynucleotide that hybridizes to the oligonucleotide; and (d) compare the amount of polynucleotide that hybridizes to the oligonucleotide to a predetermined cut-off value, and therefrom determining the presence of the cancer in the patient.
 15. A diagnostic kit comprising at least one oligonucleotide according to claim
 8. 16. A diagnostic kit comprising at least one antibody according to claim 5 and a detection reagent, wherein the detection reagent comprises a reporter group.
 17. A method for inhibiting the development of a cancer in a patient, comprising the steps of: (a) incubating CD4+ and/or CD8+ T cells isolated from a patient with at least one component selected from the group consisting of: (i) polypeptides according to claim 2; (ii) polynucleotides according to claim 1; and (iii) antigen presenting cells that express a polypeptide of claim 2, such that T cell proliferate; (b) administering to the patient an effective amount of the proliferated T cells, and thereby inhibiting the development of a cancer in the patient. 